Regression: Difference between revisions

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== Coefficient of determination ''R''<sup>2</sup> ==
== Coefficient of determination ''R''<sup>2</sup> ==
* Relationship in the simple linear regression (intercept is included)
:[[File:R-squared.png|250px]]
* https://en.wikipedia.org/wiki/Coefficient_of_determination.  
* https://en.wikipedia.org/wiki/Coefficient_of_determination.  
** ''R''<sup>2</sup> is expressed as the ratio of the explained variance to the total variance.
** ''R''<sup>2</sup> is expressed as the ratio of the explained variance to the total variance.
** It is a statistical measure of how well the regression predictions approximate the real data points.
** It is a statistical measure of how well the regression predictions approximate the real data points.
** See the wikipedia page for a list of caveats of ''R''<sup>2</sup> including '''correlation does not imply causation'''.
** See the wikipedia page for a list of caveats of ''R''<sup>2</sup> including '''correlation does not imply causation'''.
* [https://twitter.com/quasilocal/status/1659085866508140544 Based on the data collected, my tennis ball will reach orbit by tomorrow]. R2=0.85 in the following example.
:[[File:R2.png|250px]]
* [https://towardsdatascience.com/avoid-r-squared-to-judge-regression-model-performance-5c2bc53c8e2e Avoid R-squared to judge regression model performance]
* [https://towardsdatascience.com/avoid-r-squared-to-judge-regression-model-performance-5c2bc53c8e2e Avoid R-squared to judge regression model performance]
** R2 = RSS/TSS (model based)
** R2 = RSS/TSS (model based)
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* [https://stackoverflow.com/a/49974541 How R2 and RMSE are calculated in cross-validation of pls R]
* [https://stackoverflow.com/a/49974541 How R2 and RMSE are calculated in cross-validation of pls R]
* [https://www.knowledgehut.com/blog/data-science/interpret-r-squared-and-goodness-fit-regression-analysis How to Interpret R Squared and Goodness of Fit in Regression Analysis]
* [https://www.knowledgehut.com/blog/data-science/interpret-r-squared-and-goodness-fit-regression-analysis How to Interpret R Squared and Goodness of Fit in Regression Analysis]
** Limitations of R-squared: R-squared does not inform if the regression model has an adequate fit or not.  
** Limitations of R-squared: '''R-squared does not inform if the regression model has an adequate fit or not'''. It can be arbitrarily low when the model is completely correct. See [https://www.r-bloggers.com/2023/11/little-useless-useful-r-functions-how-to-make-r-squared-useless/ How to make R-squared useless].
** Low R-squared and High R-squared values. A regression model with high R2  value can lead to – as the statisticians call it – '''specification bias'''. See [https://blog.minitab.com/en/adventures-in-statistics-2/regression-analysis-how-do-i-interpret-r-squared-and-assess-the-goodness-of-fit an example].
** Low R-squared and High R-squared values. A regression model with high R2  value can lead to – as the statisticians call it – '''specification bias'''. See [https://blog.minitab.com/en/adventures-in-statistics-2/regression-analysis-how-do-i-interpret-r-squared-and-assess-the-goodness-of-fit an example].
* [https://statisticsbyjim.com/regression/r-squared-too-high/ Five Reasons Why Your R-squared can be Too High]
* [https://statisticsbyjim.com/regression/r-squared-too-high/ Five Reasons Why Your R-squared can be Too High]
** R-squared is a biased estimate. R-squared estimates tend to be greater than the correct population value.  
** R-squared is a biased estimate. R-squared estimates tend to be greater than the correct population value.  
** Overfitting your model. This problem occurs when the model is too complex.  
** Overfitting your model. This problem occurs when the model is too complex.  
::<syntaxhighlight lang='r'>
library(ggplot2)
set.seed(123)
x <- 1:100
y <- x + rnorm(100, sd = 10)
model1 <- lm(y ~ x)
summary(model1)$r.squared  # 0.914
# Now, let's add some noise variables
noise <- matrix(rnorm(100*1000), ncol = 1000)
model2 <- lm(y ~ x + noise)
summary(model2)$r.squared  # 1
</syntaxhighlight>
** Data mining and chance correlations. Multiple hypotheses.
** Data mining and chance correlations. Multiple hypotheses.
** Trends in Panel (Time Series) Data
** Trends in Panel (Time Series) Data
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lm(y~ x1 + x4) |> summary()  # x4 coef not defined because of singularities
lm(y~ x1 + x4) |> summary()  # x4 coef not defined because of singularities
lm(y~ x4 + x1) |> summary()  # x1 coef not defined because of singularities
lm(y~ x4 + x1) |> summary()  # x1 coef not defined because of singularities
</pre>
Consider lasso
<pre>
fit <- cv.glmnet(x=cbind(x1, x3, matrix(rnorm(n*10), nr=n)), y=y)
coefficients(fit, s = "lambda.min")
# 13 x 1 sparse Matrix of class "dgCMatrix"
#                      s1
# (Intercept) 0.002797165
# x1          0.970839175
# x3          .         
#            .         
fit <- cv.glmnet(x=cbind(x1, x4, matrix(rnorm(n*10), nr=n)), y=y)
coefficients(fit, s = "lambda.min")
# 13 x 1 sparse Matrix of class "dgCMatrix"
#                      s1
# (Intercept) 2.797165e-03
# x1          9.708392e-01
# x4          6.939215e-18
#            . 
fit <- cv.glmnet(x=cbind(x4, x1, matrix(rnorm(n*10), nr=n)), y=y)
coefficients(fit, s = "lambda.min")
# 13 x 1 sparse Matrix of class "dgCMatrix"
#                      s1
# (Intercept) 2.797165e-03
# x4          9.708392e-01
# x1          6.93 9215e-18
#            . 
</pre>
</pre>
<li>[https://www.statology.org/r-not-defined-because-of-singularities/ How to Fix in R: not defined because of singularities]
<li>[https://www.statology.org/r-not-defined-because-of-singularities/ How to Fix in R: not defined because of singularities]
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== Marginal effects ==
== Marginal effects ==
[https://vincentarelbundock.github.io/marginaleffects/ The '''marginaleffects''' package for R]. Compute and plot adjusted predictions, contrasts, marginal effects, and marginal means for 69 classes of statistical models in R. Conduct linear and non-linear hypothesis tests using the delta method.
* [https://cran.r-project.org/web/packages/marginaleffects/index.html CRAN], https://marginaleffects.com/
* [https://vincentarelbundock.github.io/marginaleffects/ The '''marginaleffects''' package for R]. Compute and plot adjusted predictions, contrasts, marginal effects, and marginal means for 69 classes of statistical models in R. Conduct linear and non-linear hypothesis tests using the delta method.
* [https://arelbundock.com/arel-bundock_user_20240709.html Slides]


== Confounders, confounding ==
== Confounders, confounding ==
* [https://www.statology.org/confounding-variable/ What is a Confounding Variable? (Definition & Example)]. Confounding variable is a variable that can affect the relationship between the two variables under study. Requirements for Confounding Variables:
** It must be '''correlated''' with the independent variable.
** It must have a '''causal relationship''' with the dependent variable.
* [https://rafalab.github.io/dsbook/association-is-not-causation.html#confounders Confounders] Introduction to Data Science by Irizarry
* [https://rafalab.github.io/dsbook/association-is-not-causation.html#confounders Confounders] Introduction to Data Science by Irizarry
** If X and Y are correlated, we call Z a '''confounder''' if changes in Z causes changes in both X and Y.
** If X and Y are correlated, we call Z a '''confounder''' if changes in Z causes changes in both X and Y.
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* [http://www.cantab.net/users/filimon/cursoFCDEF/will/logistic_confound.pdf Logistic Regression: Confounding and Colinearity]
* [http://www.cantab.net/users/filimon/cursoFCDEF/will/logistic_confound.pdf Logistic Regression: Confounding and Colinearity]
* [https://stats.stackexchange.com/questions/192591/identifying-a-confounder?rq=1 Identifying a confounder]
* [https://stats.stackexchange.com/questions/192591/identifying-a-confounder?rq=1 Identifying a confounder]
** [https://support.bioconductor.org/p/9157469/ Using a change in a continuous explanatory variable to test changes in gene expression with limma]. ''If the second model gives just as much DE as the first, then that is evidence that expression changes between visits are largely explained by the weight loss.''
* [https://stats.stackexchange.com/questions/38326/is-it-possible-to-have-a-variable-that-acts-as-both-an-effect-modifier-and-a-con Is it possible to have a variable that acts as both an effect modifier and a confounder?]
* [https://stats.stackexchange.com/questions/38326/is-it-possible-to-have-a-variable-that-acts-as-both-an-effect-modifier-and-a-con Is it possible to have a variable that acts as both an effect modifier and a confounder?]
* [https://stats.stackexchange.com/questions/34644/which-test-to-use-to-check-if-a-possible-confounder-impacts-a-0-1-result Which test to use to check if a possible confounder impacts a 0 / 1 result?]
* [https://stats.stackexchange.com/questions/34644/which-test-to-use-to-check-if-a-possible-confounder-impacts-a-0-1-result Which test to use to check if a possible confounder impacts a 0 / 1 result?]
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* [https://davidlindelof.com/no-you-have-not-controlled-for-confounders/ No, you have not controlled for confounders]
* [https://davidlindelof.com/no-you-have-not-controlled-for-confounders/ No, you have not controlled for confounders]
* [https://stats.stackexchange.com/questions/558403/visual-demonstration-of-residual-confounding Visual Demonstration of Residual Confounding]. Don't dichotomize a continuous variable.
* [https://stats.stackexchange.com/questions/558403/visual-demonstration-of-residual-confounding Visual Demonstration of Residual Confounding]. Don't dichotomize a continuous variable.
* See [[T-test#Randomized_block_design|Randomized block design]]
* [https://www.r-bloggers.com/2023/06/simulating-confounders-colliders-and-mediators-by-ellis2013nz/ Simulating confounders, colliders and mediators]
* Age is a confounder for some disease.
** [https://sphweb.bumc.bu.edu/otlt/MPH-Modules/BS/BS704-EP713_Confounding-EM/BS704-EP713_Confounding-EM3.html Conditions Necessary for Confounding]
** [https://sphweb.bumc.bu.edu/otlt/MPH-Modules/BS/BS704-EP713_Confounding-EM/BS704-EP713_Confounding-EM2.html What is Confounding?]
** [https://pubmed.ncbi.nlm.nih.gov/2658321/ Age: a truly confounding variable]
** [https://quantifyinghealth.com/confounding-examples/ 5 Real-World Examples of Confounding (With References)]
=== Simulated data ===
Question: gene expression ~ age + condition (condition is significant) but gene expression ~ condition (condition is not significant). Releted post: [https://support.bioconductor.org/p/9160061/ Highly DE genes but small count difference within conditions].
Possible Explanation
# '''Confounding Variable''': Age might be a confounding variable, meaning it influences both gene expression and condition. When you include age, you control for its effect, which clarifies the relationship between condition and gene expression.
# '''Interaction Effect''': There might be an interaction between age and condition. In the full model, the combined effect of age and condition provides a clearer picture of how condition affects gene expression.
# '''Multicollinearity''': It could also indicate multicollinearity, where age and condition are correlated. Including both variables might change the significance levels.
Simulated data
<ul>
<li>Confounding only (covariates).
<pre>
# Simulate data
n <- 100
age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
# Influence condition by age: older individuals more likely to have condition
condition <- ifelse(age > 50, 1, 0)
# Simulate gene expression with confounding but no interaction or multicollinearity
expression <- 5 + 0.3*age + 2*condition + rnorm(n)
# Create data frame
df <- data.frame(age, condition, expression)
</pre>
<li>Interaction only
<pre>
# Set seed for reproducibility
set.seed(123)
# Simulate data
n <- 100
age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
condition <- rbinom(n, 1, 0.5)      # Binary variable for condition
# Simulate gene expression with interaction, no confounding, no multicollinearity
expression <- 5 + 0.3*age + 2*condition + 0.5*age*condition + rnorm(n)
# Create data frame
df <- data.frame(age, condition, expression)
</pre>
<li>multicollinearity only (covariates)
<pre>
# Set seed for reproducibility
set.seed(123)
# Simulate data
n <- 100
age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
# Create a multicollinear variable that is highly correlated with age
age_collinear <- age + rnorm(n, mean = 0, sd = 2)
# Binary condition variable, independent of age
condition <- rbinom(n, 1, 0.5)
# Simulate gene expression with no confounding or interaction but with multicollinearity
expression <- 5 + 0.3*age + 0.3*age_collinear + 2*condition + rnorm(n)
# Create data frame
df <- data.frame(age, age_collinear, condition, expression)
# Check multicollinearity
library(car)
vif(lm(expression ~ age + age_collinear + condition, data = df))
# A VIF value above 10 generally indicates high multicollinearity,
# but even values above 5 might be concerning.
</pre>
<li>Everything
<pre>
# Load necessary library
library(dplyr)
# Set seed for reproducibility
set.seed(123)
# Simulate data
n <- 100
age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
# Influence condition by age: older individuals more likely to have condition
condition <- ifelse(age > 50, 1, 0) 
# Create a multicollinear variable that is highly correlated with age
age_collinear <- age + rnorm(n, mean = 0, sd = 2)
# Simulate gene expression with confounding, multicollinearity, and interaction
expression <- 5 + 0.3*age + 0.3*age_collinear + 2*condition + 0.5*age*condition + rnorm(n)
# Create data frame
df <- data.frame(age, age_collinear, condition, expression)
# Summary of data
summary(df)
# Check multicollinearity
library(car)
vif(lm(expression ~ age + age_collinear + condition, data = df))
</pre>
</ul>
Plotting
<ul>
<li>Stratified Scatter Plot
{{Pre}}
plot(df$age, df$expression, col=as.factor(df$condition), pch=16,
    main="Stratified Plot: Age vs. Expression by Condition",
    xlab="Age", ylab="Gene Expression")
legend("topright", legend=levels(as.factor(df$condition)),
      col=1:length(levels(as.factor(df$condition))),
      pch=16)
</pre>
<li>Pair Plot
{{Pre}}
pairs(~expression + age + condition, data=df,
      main="Pair Plot: Expression, Age, Condition",
      col=as.factor(df$condition), pch=16)
</pre>
</ul>


== Confidence interval vs prediction interval ==
== Confidence interval vs prediction interval ==
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* [https://www.business-science.io/r/2021/07/13/easystats-performance-check-model.html easystats: Quickly investigate model performance]
* [https://www.business-science.io/r/2021/07/13/easystats-performance-check-model.html easystats: Quickly investigate model performance]
* [https://finnstats.com/index.php/2021/11/17/homoscedasticity-in-regression-analysis/ Homoscedasticity in Regression Analysis]
* [https://finnstats.com/index.php/2021/11/17/homoscedasticity-in-regression-analysis/ Homoscedasticity in Regression Analysis]
* [https://www.r-bloggers.com/2023/12/exploring-variance-inflation-factor-vif-in-r-a-practical-guide/ Exploring Variance Inflation Factor (VIF) in R: A Practical Guide].


== Linear regression with Map Reduce ==
== Linear regression with Map Reduce ==
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* [https://en.wikipedia.org/wiki/Q%E2%80%93Q_plot Q-Q plot]
* [https://en.wikipedia.org/wiki/Q%E2%80%93Q_plot Q-Q plot]
* [https://www.tjmahr.com/quantile-quantile-plots-from-scratch/ Q-Q Plots and Worm Plots from Scratch]
* [https://www.tjmahr.com/quantile-quantile-plots-from-scratch/ Q-Q Plots and Worm Plots from Scratch]
== Added variable plots ==
[https://www.spsanderson.com/steveondata/posts/2023-10-05/index.html Added Variable Plots/partial-regression plots]


== Generalized least squares ==
== Generalized least squares ==
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[https://rileyking.netlify.app/post/linear-regression-is-smarter-than-i-thought-estimating-effect-sizes-for-variables-in-r/ Trying to Trick Linear Regression - Estimating Coefficients for Variables in R]
[https://rileyking.netlify.app/post/linear-regression-is-smarter-than-i-thought-estimating-effect-sizes-for-variables-in-r/ Trying to Trick Linear Regression - Estimating Coefficients for Variables in R]


== How to interpret the interaction term ==
== Interaction term ==
[https://stats.stackexchange.com/a/56882 how to interpret the interaction term in lm formula in R?] If both x1 and x2 are numerical, then x1:x2 is actually x1*x2 in computation. That is y ~ x1 + x2 + x1:x2 is equivalent to y ~ x1 + x2 + x3 where x3 = x1*x2. The cross is literally the two terms multiplied -- interpretation will largely depend on whether var1 and var2 are both continuous (quite hard to interpret, in my opinion) or whether one of these is e.g. binary categorical (easier to consider.)  
* [https://stats.stackexchange.com/a/56882 how to interpret the interaction term in lm formula in R?] If both x1 and x2 are numerical, then x1:x2 is actually x1*x2 in computation. That is y ~ x1 + x2 + x1:x2 is equivalent to y ~ x1 + x2 + x3 where x3 = x1*x2. The cross is literally the two terms multiplied -- interpretation will largely depend on whether var1 and var2 are both continuous (quite hard to interpret, in my opinion) or whether one of these is e.g. binary categorical (easier to consider.)
* [https://onlinelibrary.wiley.com/doi/10.1002/bimj.202300069 The marginality principle revisited: Should “higher-order” terms always be accompanied by “lower-order” terms in regression analyses?] 2023
 
== Without intercept ==
<pre>
lm(formula = y ~ x1 + x2 -1)
# or
lm(formula = y ~ x1 + x2 +0)
</pre>


== Intercept only model and cross-validation ==
== Intercept only model and cross-validation ==
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= Logistic regression =
= Logistic regression =
<ul>
<ul>
<li>[https://youtu.be/kkN9VtG26Pk 5個方式超越二元對立]
<li>https://en.wikipedia.org/wiki/Logistic_regression </li>
# 一切都是遊戲
# 練習寬恕
# 不評判 感受一切
# 信任直覺(高我)
# 親修實證
<li>[https://stats.stackexchange.com/questions/159110/logistic-regression-or-t-test Logistic regression or T test?]. [https://stats.stackexchange.com/questions/41320/choosing-between-logistic-regression-and-mann-whitney-t-tests Choosing between logistic regression and Mann Whitney/t-tests]
<li>[https://stats.stackexchange.com/questions/159110/logistic-regression-or-t-test Logistic regression or T test?]. [https://stats.stackexchange.com/questions/41320/choosing-between-logistic-regression-and-mann-whitney-t-tests Choosing between logistic regression and Mann Whitney/t-tests]
* The t-test is not significant but the logistic regression is
* The t-test is not significant but the logistic regression is
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</pre>
</pre>
[[File:LogisticFail.svg|200px]]
[[File:LogisticFail.svg|200px]]
<li>[https://www.spsanderson.com/steveondata/posts/2023-10-26/index.html Plotting a Logistic Regression In Base R]
<li>[https://mgimond.github.io/Stats-in-R/Logistic.html Logistic regression in R]. Assessing the fit with a pseudo R2. Alternative pseudo R2. Assessing the significance. </li>
<li>[https://mgimond.github.io/Stats-in-R/Logistic.html Logistic regression in R]. Assessing the fit with a pseudo R2. Alternative pseudo R2. Assessing the significance. </li>
<li>[https://www.statology.org/plot-logistic-regression-in-r/ How to Plot a Logistic Regression Curve in R] Simple model.
<li>[https://www.statology.org/plot-logistic-regression-in-r/ How to Plot a Logistic Regression Curve in R] Simple model.
<li>[https://blogs.uoregon.edu/rclub/2016/04/05/plotting-your-logistic-regression-models/ Plotting the results of your logistic regression Part 1: Continuous by categorical interaction]. Multivariate model.
<li>[https://blogs.uoregon.edu/rclub/2016/04/05/plotting-your-logistic-regression-models/ Plotting the results of your logistic regression Part 1: Continuous by categorical interaction]. Multivariate model.
<li>[https://pacha.dev/blog/2022/07/18/generalized-linear-models-part-i-the-logistic-model/ Generalized Linear Models, Part I: The Logistic Model], odds ratio, hypothesis testing, change of the reference factor
<li>Logistic regression '''log odds''' log(p/(1-p)) = beta * X </li>
<li>logit function '''f(x) = logit(x) = 1 / (1+exp(-x))''' and we model the response Y by f(b0 + b1*x).</li>
<li>[https://www.sciencedirect.com/science/article/pii/S0895435623001890 Poor handling of continuous predictors in clinical prediction models using logistic regression: a systematic review] Ma 2023
<li>[https://youtu.be/kkN9VtG26Pk 5個方式超越二元對立]
# 一切都是遊戲
# 練習寬恕
# 不評判 感受一切
# 信任直覺(高我)
# 親修實證
<li>[https://www.r-bloggers.com/2024/01/binary-logistic-regression-in-r/ Binary logistic regression in R]. Univariate, multivariate, interaction, model selection, AUC, reporting results (Odds ratio plot from the [https://finalfit.org/ finalfit] package).
</ul>
== Interpretation ==
<ul>
<li>Logistic regressions is to model the '''log odds''' of an event, rather than the probability of an event, based on a linear combination of predictor variables. log(p/(1-p)) = beta*x.
<li>[https://www.r-bloggers.com/2024/04/logistic-regression-is-not-advanced-machine-learning-or-artificial-intelligence/ Logistic regression is not advanced ‘machine learning’ or ‘artificial intelligence’]. It is possible to obtain the same coefficients from the glm() function by transforming the data following the Binomial regression “recipe” and then using lm() repeated times until reaching convergence.
<li>[https://www.r-bloggers.com/2023/11/odds-are-youre-using-probabilities-to-describe-event-outcomes/ Odds Are You’re Using Probabilities to Describe Event Outcomes]
<li>[https://www.stata.com/support/faqs/statistics/odds-ratio-versus-odds/ The difference between odds and odds ratio in logistic regression].
* '''Odds of some event''' = p/(1-p) = exp(Xb)
* '''Odds ratio''' for variable X = Odds1/Odds2 = odds(b(X+1)) / odds(bX) = exp(b(X+1)) / exp(Xb) = exp(b). This interpretation mainly applies to binary predictors.
* If the odds ratio is greater than 1, then the independent variable is positively associated with the dependent variable. This means that an increase in the independent variable will lead to an increase in the odds of the dependent variable occurring.
* If the odds ratio is less than 1, then the independent variable is negatively associated with the dependent variable. This means that an increase in the independent variable will lead to a decrease in the odds of the dependent variable occurring.
<li>[https://www.statology.org/interpret-logistic-regression-coefficients/ How to Interpret Logistic Regression Coefficients (With Example)] including binary predictor and continuous predictor variable. ''There is no need to use the convoluted term 'odds ratio' ''.
* <math>e^\beta</math> = '''Average Change'''(division) in '''Odds of an event''' (Odds1 / Odds2) for every one-unit increase of the predictor.
* β = Average Change in '''Log Odds''' of Response Variable
* Binary predictor variable case (female/male).
** If <math>e^\beta = 0.57</math>, it means males have 0.57 times the '''odds of''' passing the exam '''relative to''' females (assuming male is coded as 1 and female as 0). We could also say that males have <math>(1 - e^{\beta}) = (1 – 0.57) =</math> 43% lower '''odds of''' passing the exam than females.
** If <math>e^\beta = 1.5</math>, it means males are 1.5 times more likely to pass the exam than females. In other words, the odds of a male passing the exam are 1.5 times the odds of a female passing the exam.
* Continuous predictor variable case (number of practice exams taken). If <math>e^\beta = e^{1.13} = 3.09</math>, it means additional practice exam is '''associated with''' a '''tripling of the odds of''' passing the final exam.
** Or each additional practice exam taken is associated with (3.09-1)*100=209% '''increase''' in the '''odds of''' passing the exam, assuming the other variables are held unchanged.
** If someone originally had a 50% chance of passing (odds of 1:1), taking one more practice exam would increase their odds to 3.09. This translates to a roughly 75.6% chance/'''probability''' of passing after taking one more exam 3.09 = p/(1-p) -> p=exp(beta)/(1+exp(beta))=3.09/(4.09)=75.6%.
* Continuous predictor variable. If <math>e^\beta = e^{-.38} = 0.68</math>, it means if the predictor variable (number of practice exams) increases by one unit, the odds of passing the exam decrease by approximately 32%.
** If someone originally had a 50% chance of passing (odds of 1:1), what would be the chance of passing an exam for taking an additional practice exam? 0.68 = p/(1-p), p=0.405. Therefore, after taking one more practice exam, the chance of passing the exam decreases to approximately 40.5%.
<li>[https://quantifyinghealth.com/interpret-logistic-regression-coefficients/ Interpret Logistic Regression Coefficients (For Beginners)].  
<li>[https://quantifyinghealth.com/interpret-logistic-regression-coefficients/ Interpret Logistic Regression Coefficients (For Beginners)].  
* Increasing the predictor by 1 unit (or going from 1 level to the next) multiplies the odds of having the outcome by exp(β).
* Increasing the predictor by 1 unit (or going from 1 level to the next) multiplies the odds of having the outcome by exp(β).
Line 439: Line 671:
* If β = 0, then exp^β =1, the smoking group has the same '''odds''' as the non-smoking group of having heart disease.
* If β = 0, then exp^β =1, the smoking group has the same '''odds''' as the non-smoking group of having heart disease.
* How to interpret the intercept? If the intercept has a negative sign: then the '''probability''' of having the outcome will be < 0.5.
* How to interpret the intercept? If the intercept has a negative sign: then the '''probability''' of having the outcome will be < 0.5.
<li>[https://towardsdatascience.com/a-simple-interpretation-of-logistic-regression-coefficients-e3a40a62e8cf A Simple Interpretation of Logistic Regression Coefficients]. logit(p) = log-odds ratio.  
<li>[https://towardsdatascience.com/a-simple-interpretation-of-logistic-regression-coefficients-e3a40a62e8cf A Simple Interpretation of Logistic Regression Coefficients].  
* A 1 unit increase in X₁ will result in b increase in the log-odds ratio of success : failure.  
* '''Odds = p/(1-p)''', p is the probability that an event occurs. For example, if you roll a six-sided die, the odds of rolling a 6 is 1 to 5 (abbreviated 1:5).
* In other words, if exp(b)=1.14, it means increasing studying hour by 1 unit will have a 14% increase in the '''odds''' of passing the exam (assuming that the variable female remains fixed) where p = the probability of passing an exam.
* logit(p) = log-odds ratio.  
* A 1 unit increase in X₁ will result in beta increase in the '''log-odds ratio''' of success : failure.  
* For a one-unit increase of the predictor variable, '''the odds of the event happening''' increase by exp(beta)
* In other words, if exp(b)=1.14, it means increasing studying hour by 1 unit will have a 14% increase in the '''odds''' of passing the exam (assuming that the variable female remains fixed) where p = the probability of passing an exam. For every one unit increase in the independent variable, the '''odds of passing the test increase by a factor of''' 1.14. In other words, if a student studies for one hour more than another student, they are 1.14 times more likely to pass the test. For example, if the probability of passing the test was initially 50%, then after 1 unit increase in study hours, '''the odds of passing the test is multiplied by''' 1.14, the new probability of passing the test would be 57% (50 * 1.14 = 57 %).
* If however exp(b)=0.68, it means for every 1 unit increase in study hours, '''the odds of passing the exam decreased by a factor''' of 0.68. For example, if the odds of passing the exam were initially 50%, then after a one-unit increase in study hours, the new odds of passing the exam would be 34% (50* * 0.68 = 34%).
 
<li>[https://www.displayr.com/how-to-interpret-logistic-regression-coefficients/ How to Interpret Logistic Regression Coefficients]
<li>[https://www.displayr.com/how-to-interpret-logistic-regression-coefficients/ How to Interpret Logistic Regression Coefficients]
<li>[https://pacha.dev/blog/2022/07/18/generalized-linear-models-part-i-the-logistic-model/ Generalized Linear Models, Part I: The Logistic Model], odds ratio, hypothesis testing, change of the reference factor
 
<li>Interpretation: consider X=(intercept, x), beta = (beta0, beta1) and assume x = 0/1. Then logit(beta0) is the percentage of positive results in Y when x = 0, and logit(beta0 + beta1) is the percentage of positive results in Y when x =1. Again, exp(beta1) is the odds ratio.  The probabilities can be predicted by using the formula 1 / (1 + exp (-(b0 + b1*x)) ) </li>
</ul>
 
== Hosmer–Lemeshow test for goodness-of-fit ==
* [https://en.wikipedia.org/wiki/Hosmer%E2%80%93Lemeshow_test Hosmer–Lemeshow test]. The example assumes there are multiple observations at each x. So the observed success rate at each x is a continuous variable, not 0/1.
* [https://rpubs.com/mbounthavong/logistic_regression_part2 Logistic regression in R - Part 2 (Goodness of fit)]
* CRAN [https://cran.r-project.org/web/packages/ResourceSelection/index.html ResourceSelection] package
 
== Multinomial logistic regression ==
* https://en.wikipedia.org/wiki/Multinomial_logistic_regression Multinomial logistic regression is a classification method that generalizes logistic regression to multiclass problems.
* Softmax
** [https://en.wikipedia.org/wiki/Softmax_function Softmax function]
** [https://deepai.org/machine-learning-glossary-and-terms/softmax-layer Applications of the Softmax Function]... ''Many multi-layer neural networks end in a penultimate layer which outputs real-valued scores that are not conveniently scaled and which may be difficult to work with. Here the softmax is very useful because it converts the scores to a normalized '''probability distribution''', which can be displayed to a user or used as input to other systems.''
** ''A softmax function is applied to the output vector to generate a probability distribution, and the '''token''' in the lexicon(dictionary) with the highest probability is the output'' from the paper [https://academic.oup.com/bioinformaticsadvances/article/3/1/vbad001/6984737 Applications of transformer-based language models in bioinformatics: a survey] 2023
 
= Generalized linear models =
<ul>
<li>[https://rdrr.io/r/stats/glm.html ?glm], [https://rdrr.io/r/stats/family.html ?family]
<li>Examples:
<pre>
glm(counts ~ outcome + treatment, family = poisson())
 
glm(Postwt ~ Prewt + Treat + offset(Prewt),
                family = gaussian, data = anorexia)
 
glm(lot1 ~ log(u), data = clotting, family = Gamma)
</pre>
<li>Summarize
{| class="wikitable" style="background-color:#F7F7F8; color:#374151;"
|- style="font-weight:bold; background-color:rgba(236, 236, 241, 0.2);"
! style="vertical-align:bottom;" | Probability Distribution
! family Parameter
! style="vertical-align:bottom;" | Typical Use Cases
! style="vertical-align:bottom;" | Default Link Function
|-
| Gaussian
| style="font-weight:bold;" | gaussian (default)
| Continuous, normally distributed data
| Identity
|-
| Binomial
| style="font-weight:bold;" | binomial
| Binary (yes/no) data or proportions
| Logit, </BR>(probit, cloglog)
|-
| Poisson
| style="font-weight:bold;" | poisson
| Count data following Poisson distribution
| Log
|-
| Gamma
| style="font-weight:bold;" | Gamma
| Continuous, positive data following gamma distribution
| Inverse
|-
| Inverse Gaussian
| style="font-weight:bold;" | inverse.gaussian
| Continuous, positive data following inverse Gaussian distribution
| 1/mu^2
|-
| Tweedie
| style="font-weight:bold;" | tweedie
| Flexible distribution for various data types
| Power value
|}
</ul>
 
== Poisson regression ==
[https://www.spsanderson.com/steveondata/posts/2023-12-19/index.html A Gentle Introduction to Poisson Regression for Count Data: School’s Out, Job Offers Incoming!]
 
= Plot =
== Nomogram ==
<ul>
<li>[https://en.wikipedia.org/wiki/Nomogram Nomogram]
<li>Components of a Nomogram:
* Axes: A nomogram consists of multiple scales, each representing a variable in the model.
* Lines: Straight lines are drawn between the scales to determine the predicted outcome.
* Points: Points are assigned to each predictor variable based on its value, and these points are summed to provide an overall score, which can then be translated into a probability of the outcome. Note, the individual data points do not have to be plotted on the nomogram itself.
 
<li>How It Works:
* Input Variables: Each input variable has its own scale on the nomogram. For example, age, tumor size, and gender might be different scales.
* Point Assignment: For each input variable, a certain number of points is assigned based on its value. These points are located on a “points” axis, which is summed up to obtain a total score.
* Outcome Probability: The total score corresponds to the probability of the event of interest (e.g., survival probability) using a separate axis.  If you wanted to assess the accuracy of a nomogram, you might create a separate '''calibration plot''' where observed outcomes (from real data) are plotted against predicted probabilities (from the nomogram).
 
<li>Simple Example: Let’s consider a simplified example where a nomogram is used to predict the probability of a disease based on two factors: Age and Blood Pressure (BP).
# Age Scale: This scale might range from 20 to 80 years.
# BP Scale: This scale might range from 100 to 180 mmHg.
 
<li>Nomogram plot <br/>
[[File:Nomogram.png|150px]]
</ul>
 
== Calibration Plot ==
Calibration plots are used to compare predicted probabilities from a model (like a logistic regression or a nomogram) with the actual observed outcomes. They help assess the accuracy of a prediction model.
 
== Decision Curve Analysis (DCA) ==
Decision curve analysis evaluates the clinical usefulness of prediction models by comparing the net benefit of using the model to make decisions at various threshold probabilities.
 
== Forest Plot ==
Forest plots are commonly used in meta-analysis to display the estimated effects from multiple studies.
 
== Logistic Regression Curve ==
In binary logistic regression, the logistic curve (or S-curve) is used to model the probability of an event occurring based on a linear combination of predictor variables.
 
== Score Plot (from Principal Component Analysis) ==
 
== Partial Dependence Plot (PDP) ==
<ul>
<li>PDPs show the relationship between a predictor variable and the predicted outcome while accounting for the average effect of other predictors in the model.
 
<li>[https://cran.r-project.org/web/packages/pdp/ CRAN], [https://github.com/bgreenwell/pdp?tab=readme-ov-file github]
* [https://journal.r-project.org/archive/2017/RJ-2017-016/index.html pdp: An R Package for Constructing Partial Dependence Plots]
 
<li>[https://christophm.github.io/interpretable-ml-book/pdp.html Interpretable Machine Learning] by Christoph Molnar
 
<li>Detailed breakdown:
* How it works: For each value of the predictor variable of interest, the PDP is calculated by averaging the model’s predictions over the range of values for the other predictor variables. This isolates the effect of the predictor variable of interest from the effects of the other predictors.
* Types of PDPs:
** Univariate PDP: Shows the effect of a single predictor variable on the prediction.
** Bivariate PDP: Shows the effect of two predictor variables together on the prediction.
 
<li>Linear regression with two predictors X1 and X2
<pre>
# Load necessary libraries
library(ggplot2)
library(gridExtra)
 
# Generate sample data
set.seed(123)
n <- 100
X1 <- rnorm(n)
X2 <- rnorm(n)
Y <- 5 + 2*X1 + 3*X2 + rnorm(n)
 
# Fit a linear regression model
model <- lm(Y ~ X1 + X2)
 
# Predict function for new data
predict_model <- function(new_data) {
  predict(model, new_data)
}
 
# Partial Dependence Plot for X1
pdp_X1 <- function(X1_values) {
  new_data <- data.frame(X1 = X1_values, X2 = mean(X2))
  predictions <- predict_model(new_data)
  data.frame(X1 = X1_values, Prediction = predictions)
}
 
# Partial Dependence Plot for X2
pdp_X2 <- function(X2_values) {
  new_data <- data.frame(X1 = mean(X1), X2 = X2_values)
  predictions <- predict_model(new_data)
  data.frame(X2 = X2_values, Prediction = predictions)
}
 
# Generate values for PDPs
X1_values <- seq(min(X1), max(X1), length.out = 100)
X2_values <- seq(min(X2), max(X2), length.out = 100)
 
# Create PDP data
pdp_X1_data <- pdp_X1(X1_values)
pdp_X2_data <- pdp_X2(X2_values)
 
# Plot PDPs
p1 <- ggplot(pdp_X1_data, aes(x = X1, y = Prediction)) +
  geom_line() +
  ggtitle("Partial Dependence Plot for X1") +
  xlab("X1") + ylab("Predicted Y")
 
p2 <- ggplot(pdp_X2_data, aes(x = X2, y = Prediction)) +
  geom_line() +
  ggtitle("Partial Dependence Plot for X2") +
  xlab("X2") + ylab("Predicted Y")
 
# Display plots
grid.arrange(p1, p2, ncol = 2)
</pre>
 
<li>Cox regression. 
* '''Risk score <math> = \exp(\beta X) </math>'''. It is closely related to the hazard function h(t|X)=h0(t)exp(b*X).
* If X=1, we obtained the HR. The '''hazard ratio (HR)''' represents the effect of a one-unit change in the predictor on the hazard.
<pre>
library(survival)
library(ggplot2)
 
set.seed(123)
n <- 200
X1 <- rnorm(n)
X2 <- rnorm(n)
time <- rexp(n, exp(0.5*X1 - 0.3*X2))
status <- sample(0:1, n, replace = TRUE)
 
# Fit the Cox model
cox_model <- coxph(Surv(time, status) ~ X1 + X2)
 
# Define the predictor range
 
# Define the range of values for X1
X1_values <- seq(min(X1), max(X1), length.out = 100)
 
# Calculate the mean of X2
X2_mean <- mean(X2)
 
# Function to compute the risk score
compute_risk_score <- function(X1_values, model, X2_mean) {
  new_data <- data.frame(X1 = X1_values, X2 = X2_mean)
  risk_score <- exp(predict(model, newdata = new_data, type = "lp")) # default
  # OR
  # risk_score <- predict(model, newdata = new_data, type = "risk") # risk score
  data.frame(X1 = X1_values, RiskScore = risk_score)
}
 
pdp_X1_data <- compute_risk_score(X1_values, cox_model, X2_mean)
 
# The plot shows how the risk score changes with the predictor X1, holding X2 constant.
# The baseline hazard function  h_0(t)  is not included in the PDP, as we are focusing
#  on the relative effects of predictors.
# Plot PDP for X1
ggplot(pdp_X1_data, aes(x = X1, y = HazardRatio)) +
  geom_line() +
  ggtitle("Partial Dependence Plot for X1 in Cox Regression") +
  xlab("X1") +
  ylab("Risk score")
</pre>
Use survival probability instead of risk score.
<pre>
# Define a function to compute survival probabilities
compute_survival_prob <- function(X1_values, model, X2_mean) {
  new_data <- data.frame(X1 = X1_values, X2 = X2_mean)
  risk_score <- exp(predict(model, newdata = new_data, type = "lp")) # default
  # OR
  # risk_score <- predict(model, newdata = new_data, type = "risk")
  survival_prob <- baseline_survival_prob ^ risk_score
  return(survival_prob)
}
 
# Approximate survival probability (assuming a fixed time t for illustration)
# You would need to adjust this based on your actual survival analysis
# For demonstration purposes, we assume baseline survival probability at time t
baseline_survival_prob <- 0.9  # S0(t)
 
# Compute survival probabilities for the range of X1 values
survival_probs <- compute_survival_prob(X1_values, cox_model, X2_mean)
 
library(ggplot2)
 
# Create a data frame for plotting
pdp_data <- data.frame(X1 = X1_values, SurvivalProbability = survival_probs)
 
# Plot the survival function vs. predictor
ggplot(pdp_data, aes(x = X1, y = SurvivalProbability)) +
  geom_line() +
  ggtitle("Partial Dependence Plot: Survival Function vs Predictor") +
  xlab("Predictor (X1)") +
  ylab("Survival Probability")
</pre>
</ul>
</ul>


= Quantile regression =
= Quantile regression =
* https://en.wikipedia.org/wiki/Quantile_regression
<ul>
* [https://insightr.wordpress.com/2019/08/13/basic-quantile-regression/ Basic Quantile Regression]
<li>Quantile regression is a type of regression analysis in which '''quantiles of the dependent variable''' (unlike traditional linear regression, which models the '''mean of the dependent variable''') are modeled as a function of independent variables. This allows for a better understanding of the distribution of the dependent variable, especially when the distribution is skewed or has outliers.
* [https://freakonometrics.hypotheses.org/59875 QUANTILE REGRESSION (HOME MADE, PART 2)]
<li>https://en.wikipedia.org/wiki/Quantile_regression
<li>[https://insightr.wordpress.com/2019/08/13/basic-quantile-regression/ Basic Quantile Regression]
<li>[https://freakonometrics.hypotheses.org/59875 QUANTILE REGRESSION (HOME MADE, PART 2)]
<pre>
library(quantreg)
set.seed(123)
x <- rnorm(100)
y <- x + rnorm(100, mean = 0, sd = 2)
y[1:10] <- y[1:10] + 10 # first 10 are outliers
 
# Fit a traditional linear regression model
fit_lm <- lm(y ~ x)
 
# Fit a quantile regression model for the 50th percentile
fit_qr <- rq(y ~ x, tau = 0.5)
 
fit_lm$coefficients
# (Intercept)          x
#  0.7961233  0.8759269
fit_qr$coefficients
# (Intercept)          x
#  0.0772395  1.0058387
 
plot(x, y)
points(x[1:10], y[1:10], col='red', pch=16)
abline(fit_lm)
abline(fit_qr, col = 'blue')
</pre>
<li>[https://www.r-bloggers.com/2023/11/navigating-quantile-regression-with-r-a-comprehensive-guide/ Navigating Quantile Regression with R: A Comprehensive Guide]
</ul>


= Isotonic regression =
= Isotonic regression =
Line 455: Line 978:
* [https://statisticaloddsandends.wordpress.com/2021/07/29/getting-predictions-from-an-isotonic-regression-model Getting predictions from an isotonic regression model]
* [https://statisticaloddsandends.wordpress.com/2021/07/29/getting-predictions-from-an-isotonic-regression-model Getting predictions from an isotonic regression model]
* [https://onlinelibrary.wiley.com/doi/abs/10.1111/biom.13511 Pool adjacent violators algorithm assisted learning with application on estimating optimal individualized treatment regimes] 2021
* [https://onlinelibrary.wiley.com/doi/abs/10.1111/biom.13511 Pool adjacent violators algorithm assisted learning with application on estimating optimal individualized treatment regimes] 2021
= Piecewise linear regression =
* [https://www.r-bloggers.com/2023/12/unraveling-patterns-a-step-by-step-guide-to-piecewise-regression-in-r/ Unraveling Patterns: A Step-by-Step Guide to Piecewise Regression in R]
* Trajectory (related to "time")
** [https://www.visualcapitalist.com/infection-trajectory-flattening-the-covid19-curve/ Infection Trajectory: See Which Countries are Flattening Their COVID-19 Curve]
** [https://magazine.jhsph.edu/2021/covid-19-how-predict-patients-trajectory Covid-19: How to Predict a Patient's Trajectory] and [https://rsconnect.biostat.jhsph.edu/covid_predict/ The COVID Inpatient Risk Calculator: CIRC]
** [https://rss.onlinelibrary.wiley.com/doi/full/10.1111/rssb.12453?campaign=woletoc Modelling the COVID-19 infection trajectory: A piecewise linear quantile trend model] 2021
** [https://www.bmj.com/content/377/bmj-2021-069676.long Trajectory of long covid symptoms after covid-19 vaccination: community based cohort study] 2022. The time series model came from this paper [https://academic.oup.com/ije/article/46/1/348/2622842 Interrupted time series regression for the evaluation of public health interventions: a tutorial] which contains R code.
= Support vector regression =
* [https://towardsdatascience.com/an-introduction-to-support-vector-regression-svr-a3ebc1672c2 An Introduction to Support Vector Regression (SVR)].
** The goal of SVR is to find a function that approximates the relationship between the input and output variables in the training data, with an acceptable amount of error. This is done by mapping the input data into a high-dimensional feature space using a '''kernel function''', and then finding a '''linear regression''' function in that space that fits the data with a specified margin of error.
** SVR has been proven to be an effective tool in real-value function estimation, and like SVM, it is characterized by the use of kernels, sparse solution, and VC control of the margin and the number of support vectors.
* [https://link.springer.com/chapter/10.1007/978-1-4302-5990-9_4 Awad] in Springer
= Model Misspecification =
* [https://vgherard.github.io/posts/2023-05-14-model-misspecification-and-linear-sandwiches/ Model Misspecification and Linear Sandwiches]
* [https://cran.r-project.org/web/packages/sandwich/index.html sandwich] package -  Robust Covariance Matrix Estimators.
== Robust regression ==
* [https://en.wikipedia.org/wiki/Robust_regression Wikipedia]. M-estimator.
* [https://www.r-bloggers.com/2023/11/understanding-and-implementing-robust-regression-in-r/ Understanding and Implementing Robust Regression in R]. MASS::rlm().
* The function allows one to fit a linear model by robust regression using an M-estimator, allowing robust inference for parameters and robust model selection. The robust fit is minimally influenced by '''outliers''' in the response variable, in the explanatory variable(s) or in both. [https://www.oreilly.com/library/view/the-r-book/9780470510247/ch010-sec020.html The R book].
* [https://developer.nvidia.com/blog/dealing-with-outliers-using-three-robust-linear-regression-models/ Dealing with Outliers Using Three Robust Linear Regression Models]
== Example 1: data with outliers ==
Below is an example where we fit the data using '''linear regression''', '''robust linear regression''' (Robust against outliers and deviations from normality), '''quantile regression''' (Estimates conditional quantiles of the response variable), '''Theil-sen regression''' (Computes the median of pairwise slopes between data points) and '''Local polynomial regression''' (non-linear relationships and adapts to local variations).
[[File:DataOutliers.png|250px]]
== Example 2: data with outliers ==
The raw data are 'recovered' from the page [https://developer.nvidia.com/blog/dealing-with-outliers-using-three-robust-linear-regression-models/ Dealing with Outliers Using Three Robust Linear Regression Models]. In this case, [https://en.wikipedia.org/wiki/Theil%E2%80%93Sen_estimator Theil-sen regression] performed better than the other methods.
[[File:DataOutliers2.png|250px]]
= Choose variables =
[https://onlinelibrary.wiley.com/doi/full/10.1002/bimj.202200209 Variable selection in linear regression models: Choosing the best subset is not always the best choice] 2023
== Stepwise selection of variables ==
[https://www.r-bloggers.com/2024/09/stepwise-selection-of-variables-in-regression-is-evil-by-ellis2013nz/ Stepwise selection of variables in regression is Evil]
= GEE/generalized estimating equations =
See [[Longitudinal#GEE/generalized_estimating_equations|Longitudinal data analysis]].
= Deming regression =
[https://en.wikipedia.org/wiki/Deming_regression Deming regression]
= Tweedie regression =
[https://freakonometrics.hypotheses.org/66791 Model selection, AIC and Tweedie regression]


= Causal inference =
= Causal inference =
Line 494: Line 1,067:
* [https://arxiv.org/abs/2107.00122v1 Assignment-Control Plots: A Visual Companion for Causal Inference Study Design], [https://www.tandfonline.com/doi/abs/10.1080/00031305.2022.2051605 The American Statistician]
* [https://arxiv.org/abs/2107.00122v1 Assignment-Control Plots: A Visual Companion for Causal Inference Study Design], [https://www.tandfonline.com/doi/abs/10.1080/00031305.2022.2051605 The American Statistician]
* [https://arxiv.org/abs/2006.11754 Regression and Causality] by Michael Schomaker
* [https://arxiv.org/abs/2006.11754 Regression and Causality] by Michael Schomaker
* [https://towardsdatascience.com/a-complete-guide-to-causal-inference-8d5aaca68a47 A Complete Guide to Causal Inference] A compilation of the issues that you kept skipping over, and how to do it right.
* [https://ruc-econ.github.io/References/Statistical_learning/Wager-Estimation%20and%20Inference%20of%20Heterogeneous%20Treatment%20Effects%20using%20Random%20Forests-2018-Journal%20of%20the%20American%20Statistical%20Association.pdf Estimation and Inference of Heterogeneous Treatment Effects using Random Forests] Wager Athey 2018. [https://github.com/susanathey/causalTree causalTree] package.
* generalized random forests [https://cran.r-project.org/web/packages/grf/index.html CRAN]. Athey, Wager, Tibshirani. 2019
* [https://youtu.be/a_CmfRjZ_oY?t=412 Modeling Heterogeneous Treatment Effects with R] (video)
* [https://solomonkurz.netlify.app/blog/2023-05-07-causal-inference-with-count-regression/ Causal inference with count regression]
* [https://www.r-bloggers.com/2023/08/introduction-to-structural-causal-modelling/ Introduction to structural causal modelling] Christopher J. Brown
= Seemingly unrelated regressions/SUR =
<ul>
<li>[https://en.wikipedia.org/wiki/Seemingly_unrelated_regressions Seemingly unrelated regressions] from wikipedia
* Advantages: The SUR model is useful when the error terms of the regression equations are correlated with each other. In this case, the ordinary least squares (OLS) estimator is inefficient and inconsistent. The SUR model can provide more efficient and consistent estimates of the regression coefficients
* Disadvantages: One disadvantage of using the SUR model is that it requires the assumption that the error terms are correlated across equations. If this assumption is not met, then the SUR model may not provide more efficient estimates than estimating each equation separately1. Another disadvantage of using the SUR model is that it can be computationally intensive and may require more time to estimate than estimating each equation separately
<li>[https://bashtage.github.io/linearmodels/system/mathematical-formula.html  Seemingly Unrelated Regression (SUR/SURE)]
<li>[https://stats.oarc.ucla.edu/r/faq/how-can-i-perform-seemingly-unrelated-regression-in-r/ How can I perform seemingly unrelated regression in R?]
* [https://cran.r-project.org/web/packages/systemfit/index.html systemfit] package
<li>[https://cran.r-project.org/web/packages/spsur/index.html spsur] package
<li>Equations for the simplest case:
:<math>
\begin{align}
y_1 &= b_1x_1 + b_2x_2 + u_1 \\
y_2 &= b_3x_1 + b_4x_2 + u_2
\end{align}
</math>
</ul>

Latest revision as of 14:40, 18 November 2024

Linear Regression

Comic

MSE

Coefficient of determination R2

  • Relationship in the simple linear regression (intercept is included)
R-squared.png
  • https://en.wikipedia.org/wiki/Coefficient_of_determination.
    • R2 is expressed as the ratio of the explained variance to the total variance.
    • It is a statistical measure of how well the regression predictions approximate the real data points.
    • See the wikipedia page for a list of caveats of R2 including correlation does not imply causation.
R2.png
library(ggplot2)
set.seed(123)
x <- 1:100
y <- x + rnorm(100, sd = 10)
model1 <- lm(y ~ x)
summary(model1)$r.squared  # 0.914

# Now, let's add some noise variables
noise <- matrix(rnorm(100*1000), ncol = 1000)
model2 <- lm(y ~ x + noise)
summary(model2)$r.squared  # 1
[math]\displaystyle{ \begin{align} R^2 &= 1 - \frac{SSE}{SST} \\ &= 1 - \frac{MSE}{Var(y)} \end{align} }[/math]

Pearson correlation and linear regression slope

[math]\displaystyle{ \begin{align} b_1 &= r \frac{S_y}{S_x} \end{align} }[/math]

where [math]\displaystyle{ S_x=\sqrt{\sum(x-\bar{x})^2} }[/math].

set.seed(1)
x <- rnorm(10); y <-rnorm(10)
coef(lm(y~x))
# (Intercept)           x
#   0.3170798  -0.5161377

cor(x, y)*sd(y)/sd(x)
# [1] -0.5161377

Different models (in R)

http://www.quantide.com/raccoon-ch-1-introduction-to-linear-models-with-r/

Factor Variables

Regression With Factor Variables

dummy.coef.lm() in R

Extracts coefficients in terms of the original levels of the coefficients rather than the coded variables.

Add Regression Line per Group to Scatterplot

How To Add Regression Line per Group to Scatterplot in ggplot2?

penguins_df %>%
  ggplot(aes(x=culmen_length_mm, 
             y=flipper_length_mm, 
             color=species))+
  geom_point()+
  geom_smooth(method="lm", se = FALSE)

model.matrix, design matrix

Contrasts in linear regression

  • Page 147 of Modern Applied Statistics with S (4th ed)
  • https://biologyforfun.wordpress.com/2015/01/13/using-and-interpreting-different-contrasts-in-linear-models-in-r/ This explains the meanings of 'treatment', 'helmert' and 'sum' contrasts.
  • A (sort of) Complete Guide to Contrasts in R by Rose Maier
    mat
    
    ##      constant NLvMH  NvL  MvH
    ## [1,]        1  -0.5  0.5  0.0
    ## [2,]        1  -0.5 -0.5  0.0
    ## [3,]        1   0.5  0.0  0.5
    ## [4,]        1   0.5  0.0 -0.5
    mat <- mat[ , -1]
    
    model7 <- lm(y ~ dose, data=data, contrasts=list(dose=mat) )
    summary(model7)
    
    ## Coefficients:
    ##             Estimate Std. Error t value Pr(>|t|)    
    ## (Intercept)  118.578      1.076 110.187  < 2e-16 ***
    ## doseNLvMH      3.179      2.152   1.477  0.14215    
    ## doseNvL       -8.723      3.044  -2.866  0.00489 ** 
    ## doseMvH       13.232      3.044   4.347 2.84e-05 ***
    
    # double check your contrasts
    attributes(model7$qr$qr)$contrasts
    ## $dose
    ##      NLvMH  NvL  MvH
    ## None  -0.5  0.5  0.0
    ## Low   -0.5 -0.5  0.0
    ## Med    0.5  0.0  0.5
    ## High   0.5  0.0 -0.5
    
    library(dplyr)
    dose.means <- summarize(group_by(data, dose), y.mean=mean(y))
    dose.means
    ## Source: local data frame [4 x 2]
    ## 
    ##   dose   y.mean
    ## 1 None 112.6267
    ## 2  Low 121.3500
    ## 3  Med 126.7839
    ## 4 High 113.5517
    
    # The coefficient estimate for the first contrast (3.18) equals the average of 
    # the last two groups (126.78 + 113.55 /2 = 120.17) minus the average of 
    # the first two groups (112.63 + 121.35 /2 = 116.99).

Multicollinearity

  • A toy example
    n <- 100
    set.seed(1)
    x1 <- rnorm(n)
    e <- rnorm(n)*.01
    y <- x1 + e
    cor(y, e)  # 0.00966967
    cor(y, x1) # 0.9999
    lm(y ~ x1) |> summary()      # p<2e-16
    
    set.seed(2)
    x2 <- x1 + rnorm(n)*.1       # x2 = x1 + noise
    cor(x1, x2)  # .99
    lm(y ~ x1 + x2) |> summary() # x2 insig
    lm(y~ x2) |> summary()       # x2 sig
    
    set.seed(3)
    x3 <- x1 + rnorm(n)*.0001    # x3 = x1 + tiny noise
    cor(x1, x3) # 1
    lm(y ~ x1 + x3) |> summary() # both insig. SURPRISE!
    lm(y ~ x1) |> summary()
    
    x4 <- x1                     # x4 is exactly equal to x1  
    lm(y~ x1 + x4) |> summary()  # x4 coef not defined because of singularities
    lm(y~ x4 + x1) |> summary()  # x1 coef not defined because of singularities
    

    Consider lasso

    fit <- cv.glmnet(x=cbind(x1, x3, matrix(rnorm(n*10), nr=n)), y=y)
    coefficients(fit, s = "lambda.min")
    # 13 x 1 sparse Matrix of class "dgCMatrix"
    #                      s1
    # (Intercept) 0.002797165
    # x1          0.970839175
    # x3          .          
    #             .          
    
    fit <- cv.glmnet(x=cbind(x1, x4, matrix(rnorm(n*10), nr=n)), y=y)
    coefficients(fit, s = "lambda.min")
    # 13 x 1 sparse Matrix of class "dgCMatrix"
    #                       s1
    # (Intercept) 2.797165e-03
    # x1          9.708392e-01
    # x4          6.939215e-18
    #             .   
    
    fit <- cv.glmnet(x=cbind(x4, x1, matrix(rnorm(n*10), nr=n)), y=y)
    coefficients(fit, s = "lambda.min")
    # 13 x 1 sparse Matrix of class "dgCMatrix"
    #                      s1
    # (Intercept) 2.797165e-03
    # x4          9.708392e-01
    # x1          6.93 9215e-18
    #             .   
    
  • How to Fix in R: not defined because of singularities
  • Multicollinearity in R
  • Detecting multicollinearity — it’s not that easy sometimes
  • alias: Find Aliases (Dependencies) In A Model
    > op <- options(contrasts = c("contr.helmert", "contr.poly"))
    > npk.aov <- aov(yield ~ block + N*P*K, npk)
    > alias(npk.aov)
    Model :
    yield ~ block + N * P * K
    
    Complete :
             (Intercept) block1 block2 block3 block4 block5 N1    P1    K1    N1:P1 N1:K1 P1:K1
    N1:P1:K1     0           1    1/3    1/6  -3/10   -1/5      0     0     0     0     0     0
    
    > options(op)
    

Exposure

https://en.mimi.hu/mathematics/exposure_variable.html

Independent variable = predictor = explanatory = exposure variable

Marginal effects

Confounders, confounding

Simulated data

Question: gene expression ~ age + condition (condition is significant) but gene expression ~ condition (condition is not significant). Releted post: Highly DE genes but small count difference within conditions.

Possible Explanation

  1. Confounding Variable: Age might be a confounding variable, meaning it influences both gene expression and condition. When you include age, you control for its effect, which clarifies the relationship between condition and gene expression.
  2. Interaction Effect: There might be an interaction between age and condition. In the full model, the combined effect of age and condition provides a clearer picture of how condition affects gene expression.
  3. Multicollinearity: It could also indicate multicollinearity, where age and condition are correlated. Including both variables might change the significance levels.

Simulated data

  • Confounding only (covariates).
    # Simulate data
    n <- 100
    age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
    
    # Influence condition by age: older individuals more likely to have condition
    condition <- ifelse(age > 50, 1, 0) 
    
    # Simulate gene expression with confounding but no interaction or multicollinearity
    expression <- 5 + 0.3*age + 2*condition + rnorm(n)
    
    # Create data frame
    df <- data.frame(age, condition, expression)
    
  • Interaction only
    # Set seed for reproducibility
    set.seed(123)
    
    # Simulate data
    n <- 100
    age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
    condition <- rbinom(n, 1, 0.5)       # Binary variable for condition
    
    # Simulate gene expression with interaction, no confounding, no multicollinearity
    expression <- 5 + 0.3*age + 2*condition + 0.5*age*condition + rnorm(n)
    
    # Create data frame
    df <- data.frame(age, condition, expression)
    
  • multicollinearity only (covariates)
    # Set seed for reproducibility
    set.seed(123)
    
    # Simulate data
    n <- 100
    age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
    # Create a multicollinear variable that is highly correlated with age
    age_collinear <- age + rnorm(n, mean = 0, sd = 2) 
    
    # Binary condition variable, independent of age
    condition <- rbinom(n, 1, 0.5)
    
    # Simulate gene expression with no confounding or interaction but with multicollinearity
    expression <- 5 + 0.3*age + 0.3*age_collinear + 2*condition + rnorm(n)
    
    # Create data frame
    df <- data.frame(age, age_collinear, condition, expression)
    
    # Check multicollinearity
    library(car)
    vif(lm(expression ~ age + age_collinear + condition, data = df))
    # A VIF value above 10 generally indicates high multicollinearity, 
    # but even values above 5 might be concerning.
    
  • Everything
    # Load necessary library
    library(dplyr)
    
    # Set seed for reproducibility
    set.seed(123)
    
    # Simulate data
    n <- 100
    age <- rnorm(n, mean = 50, sd = 10)  # Continuous variable for age
    # Influence condition by age: older individuals more likely to have condition
    condition <- ifelse(age > 50, 1, 0)  
    
    # Create a multicollinear variable that is highly correlated with age
    age_collinear <- age + rnorm(n, mean = 0, sd = 2)
    
    # Simulate gene expression with confounding, multicollinearity, and interaction
    expression <- 5 + 0.3*age + 0.3*age_collinear + 2*condition + 0.5*age*condition + rnorm(n)
    
    # Create data frame
    df <- data.frame(age, age_collinear, condition, expression)
    
    # Summary of data
    summary(df)
    
    # Check multicollinearity
    library(car)
    vif(lm(expression ~ age + age_collinear + condition, data = df))
    

Plotting

  • Stratified Scatter Plot
    plot(df$age, df$expression, col=as.factor(df$condition), pch=16, 
         main="Stratified Plot: Age vs. Expression by Condition", 
         xlab="Age", ylab="Gene Expression")
    legend("topright", legend=levels(as.factor(df$condition)), 
           col=1:length(levels(as.factor(df$condition))), 
           pch=16)
    
  • Pair Plot
    pairs(~expression + age + condition, data=df, 
          main="Pair Plot: Expression, Age, Condition", 
          col=as.factor(df$condition), pch=16)
    

Confidence interval vs prediction interval

Confidence intervals tell you about how well you have determined the mean E(Y). Prediction intervals tell you where you can expect to see the next data point sampled. That is, CI is computed using Var(E(Y|X)) and PI is computed using Var(E(Y|X) + e).

Homoscedasticity, Heteroskedasticity, Check model for (non-)constant error variance

Linear regression with Map Reduce

https://freakonometrics.hypotheses.org/53269

Relationship between multiple variables

Visualizing the relationship between multiple variables

Model fitting evaluation, Q-Q plot

Added variable plots

Added Variable Plots/partial-regression plots

Generalized least squares

Reduced rank regression

Singular value decomposition

  • Moore-Penrose matrix inverse in R
    > a = matrix(c(2, 3), nr=1)
    > MASS::ginv(a) * 8 
             [,1]
    [1,] 1.230769
    [2,] 1.846154  
    # Same solution as matlab lsqminnorm(A,b)
    
    > a %*% MASS::ginv(a)
         [,1]
    [1,]    1
    > a %*% MASS::ginv(a) %*% a
         [,1] [,2]
    [1,]    2    3
    > MASS::ginv   # view the source code
    

Mahalanobis distance and outliers detection

Mahalanobis distance

  • The Mahalanobis distance is a measure of the distance between a point P and a distribution D
  • It is a multi-dimensional generalization of the idea of measuring how many standard deviations away P is from the mean of D.
  • The Mahalanobis distance is thus unitless and scale-invariant, and takes into account the correlations of the data set.
  • Distance is not always what it seems

performance::check_outliers() Outliers detection (check for influential observations)

How to Calculate Mahalanobis Distance in R

set.seed(1234)
x <- matrix(rnorm(200), nc=10)
x0 <- rnorm(10)
mu <- colMeans(x)
mahalanobis(x0, colMeans(x), var(x)) # 17.76527
t(x0-mu) %*% MASS::ginv(var(x)) %*% (x0-mu) # 17.76527

# Variance is not full rank
x <- matrix(rnorm(200), nc=20)
x0 <- rnorm(20)
mu <- colMeans(x)
t(x0-mu) %*% MASS::ginv(var(x)) %*% (x0-mu)
mahalanobis(x0, colMeans(x), var(x))
# Error in solve.default(cov, ...) : 
#   system is computationally singular: reciprocal condition number = 1.93998e-19

Type 1 error

Linear Regression And Type I Error

More Data Can Hurt for Linear Regression

Sometimes more data can hurt!

Estimating Coefficients for Variables in R

Trying to Trick Linear Regression - Estimating Coefficients for Variables in R

Interaction term

Without intercept

lm(formula = y ~ x1 + x2 -1)
# or
lm(formula = y ~ x1 + x2 +0)

Intercept only model and cross-validation

n <- 20
set.seed(1)
x <- rnorm(n)
y <- 2*x + .5*rnorm(n)
plot(x, y)
df <- data.frame(x=x, y=y)
pred <- double(n)
for(i in 1:n) {
  fit <- lm(y ~ 1, data = df[-i, ])
  pred[i] <- predict(fit, df[i, ])
}
plot(y, pred)
cor(y, pred) # -1

How about 1000 simulated data?

foo <- function(n=3, debug=F) {
  x <- rnorm(n)
  y <- 2*x + .5*rnorm(n)
  df <- data.frame(x=x, y=y)
  pred <- double(n)
  for(i in 1:n) {
    fit <- lm(y ~ 1, data = df[-i, ])
    pred[i] <- predict(fit, df[i, ])
  }
  if (debug) {
    cat("num=", n*sum(y*pred)-sum(pred)*sum(y), "\n")
    cat("denom=", sqrt(n*sum(y**2) - sum(y)^2)*sqrt(n*sum(pred**2)-sum(pred)^2), "\n")
    invisible(list(y=y, pred=pred, cor=cor(y, pred)))
  } else {
    cor(y, pred)
  }
}

o <- replicate(1000, foo(n=10))
range(o) # [1] -1 -1
all.equal(o, rep(-1, 1000)) # TRUE

Note the property will not happen in k-fold CV (not LOOCV)

n <- 20; nfold <- 5
set.seed(1)
x <- rnorm(n)
y <- 2*x + .5*rnorm(n)
#plot(x, y)
df <- data.frame(x=x, y=y)
set.seed(1)
folds <- split(sample(1:n), rep(1:nfold, length = n))
pred <- double(n)
for(i in 1:nfold) {
  fit <- lm(y ~ 1, data = df[-folds[[i]], ])
  pred[folds[[i]]] <- predict(fit, df[folds[[i]], ])
}
plot(y, pred)
cor(y, pred) # -0.6696743

See also

lm.fit and multiple responses/genes

Logistic regression

Interpretation

  • Logistic regressions is to model the log odds of an event, rather than the probability of an event, based on a linear combination of predictor variables. log(p/(1-p)) = beta*x.
  • Logistic regression is not advanced ‘machine learning’ or ‘artificial intelligence’. It is possible to obtain the same coefficients from the glm() function by transforming the data following the Binomial regression “recipe” and then using lm() repeated times until reaching convergence.
  • Odds Are You’re Using Probabilities to Describe Event Outcomes
  • The difference between odds and odds ratio in logistic regression.
    • Odds of some event = p/(1-p) = exp(Xb)
    • Odds ratio for variable X = Odds1/Odds2 = odds(b(X+1)) / odds(bX) = exp(b(X+1)) / exp(Xb) = exp(b). This interpretation mainly applies to binary predictors.
    • If the odds ratio is greater than 1, then the independent variable is positively associated with the dependent variable. This means that an increase in the independent variable will lead to an increase in the odds of the dependent variable occurring.
    • If the odds ratio is less than 1, then the independent variable is negatively associated with the dependent variable. This means that an increase in the independent variable will lead to a decrease in the odds of the dependent variable occurring.
  • How to Interpret Logistic Regression Coefficients (With Example) including binary predictor and continuous predictor variable. There is no need to use the convoluted term 'odds ratio' .
    • [math]\displaystyle{ e^\beta }[/math] = Average Change(division) in Odds of an event (Odds1 / Odds2) for every one-unit increase of the predictor.
    • β = Average Change in Log Odds of Response Variable
    • Binary predictor variable case (female/male).
      • If [math]\displaystyle{ e^\beta = 0.57 }[/math], it means males have 0.57 times the odds of passing the exam relative to females (assuming male is coded as 1 and female as 0). We could also say that males have [math]\displaystyle{ (1 - e^{\beta}) = (1 – 0.57) = }[/math] 43% lower odds of passing the exam than females.
      • If [math]\displaystyle{ e^\beta = 1.5 }[/math], it means males are 1.5 times more likely to pass the exam than females. In other words, the odds of a male passing the exam are 1.5 times the odds of a female passing the exam.
    • Continuous predictor variable case (number of practice exams taken). If [math]\displaystyle{ e^\beta = e^{1.13} = 3.09 }[/math], it means additional practice exam is associated with a tripling of the odds of passing the final exam.
      • Or each additional practice exam taken is associated with (3.09-1)*100=209% increase in the odds of passing the exam, assuming the other variables are held unchanged.
      • If someone originally had a 50% chance of passing (odds of 1:1), taking one more practice exam would increase their odds to 3.09. This translates to a roughly 75.6% chance/probability of passing after taking one more exam 3.09 = p/(1-p) -> p=exp(beta)/(1+exp(beta))=3.09/(4.09)=75.6%.
    • Continuous predictor variable. If [math]\displaystyle{ e^\beta = e^{-.38} = 0.68 }[/math], it means if the predictor variable (number of practice exams) increases by one unit, the odds of passing the exam decrease by approximately 32%.
      • If someone originally had a 50% chance of passing (odds of 1:1), what would be the chance of passing an exam for taking an additional practice exam? 0.68 = p/(1-p), p=0.405. Therefore, after taking one more practice exam, the chance of passing the exam decreases to approximately 40.5%.
  • Interpret Logistic Regression Coefficients (For Beginners).
    • Increasing the predictor by 1 unit (or going from 1 level to the next) multiplies the odds of having the outcome by exp(β).
    • exp^β is the odds ratio that associates smoking to the risk of heart disease.
    • If exp^β = exp^0.38 = 1.46, the smoking group has a 1.46 times the odds of the non-smoking group of having heart disease.
    • The smoking group has 46% (1.46 – 1 = 0.46) more odds of having heart disease than the non-smoking group.
    • If β = – 0.38, then exp^β = 0.68 and the interpretation becomes: smoking is associated with a 32% (1 – 0.68 = 0.32) reduction in the relative risk of heart disease.
    • If β = 0, then exp^β =1, the smoking group has the same odds as the non-smoking group of having heart disease.
    • How to interpret the intercept? If the intercept has a negative sign: then the probability of having the outcome will be < 0.5.
  • A Simple Interpretation of Logistic Regression Coefficients.
    • Odds = p/(1-p), p is the probability that an event occurs. For example, if you roll a six-sided die, the odds of rolling a 6 is 1 to 5 (abbreviated 1:5).
    • logit(p) = log-odds ratio.
    • A 1 unit increase in X₁ will result in beta increase in the log-odds ratio of success : failure.
    • For a one-unit increase of the predictor variable, the odds of the event happening increase by exp(beta)
    • In other words, if exp(b)=1.14, it means increasing studying hour by 1 unit will have a 14% increase in the odds of passing the exam (assuming that the variable female remains fixed) where p = the probability of passing an exam. For every one unit increase in the independent variable, the odds of passing the test increase by a factor of 1.14. In other words, if a student studies for one hour more than another student, they are 1.14 times more likely to pass the test. For example, if the probability of passing the test was initially 50%, then after 1 unit increase in study hours, the odds of passing the test is multiplied by 1.14, the new probability of passing the test would be 57% (50 * 1.14 = 57 %).
    • If however exp(b)=0.68, it means for every 1 unit increase in study hours, the odds of passing the exam decreased by a factor of 0.68. For example, if the odds of passing the exam were initially 50%, then after a one-unit increase in study hours, the new odds of passing the exam would be 34% (50* * 0.68 = 34%).
  • How to Interpret Logistic Regression Coefficients
  • Interpretation: consider X=(intercept, x), beta = (beta0, beta1) and assume x = 0/1. Then logit(beta0) is the percentage of positive results in Y when x = 0, and logit(beta0 + beta1) is the percentage of positive results in Y when x =1. Again, exp(beta1) is the odds ratio. The probabilities can be predicted by using the formula 1 / (1 + exp (-(b0 + b1*x)) )

Hosmer–Lemeshow test for goodness-of-fit

Multinomial logistic regression

Generalized linear models

  • ?glm, ?family
  • Examples:
    glm(counts ~ outcome + treatment, family = poisson())
    
    glm(Postwt ~ Prewt + Treat + offset(Prewt),
                    family = gaussian, data = anorexia)
    
    glm(lot1 ~ log(u), data = clotting, family = Gamma)
    
  • Summarize
    Probability Distribution family Parameter Typical Use Cases Default Link Function
    Gaussian gaussian (default) Continuous, normally distributed data Identity
    Binomial binomial Binary (yes/no) data or proportions Logit,
    (probit, cloglog)
    Poisson poisson Count data following Poisson distribution Log
    Gamma Gamma Continuous, positive data following gamma distribution Inverse
    Inverse Gaussian inverse.gaussian Continuous, positive data following inverse Gaussian distribution 1/mu^2
    Tweedie tweedie Flexible distribution for various data types Power value

Poisson regression

A Gentle Introduction to Poisson Regression for Count Data: School’s Out, Job Offers Incoming!

Plot

Nomogram

  • Nomogram
  • Components of a Nomogram:
    • Axes: A nomogram consists of multiple scales, each representing a variable in the model.
    • Lines: Straight lines are drawn between the scales to determine the predicted outcome.
    • Points: Points are assigned to each predictor variable based on its value, and these points are summed to provide an overall score, which can then be translated into a probability of the outcome. Note, the individual data points do not have to be plotted on the nomogram itself.
  • How It Works:
    • Input Variables: Each input variable has its own scale on the nomogram. For example, age, tumor size, and gender might be different scales.
    • Point Assignment: For each input variable, a certain number of points is assigned based on its value. These points are located on a “points” axis, which is summed up to obtain a total score.
    • Outcome Probability: The total score corresponds to the probability of the event of interest (e.g., survival probability) using a separate axis. If you wanted to assess the accuracy of a nomogram, you might create a separate calibration plot where observed outcomes (from real data) are plotted against predicted probabilities (from the nomogram).
  • Simple Example: Let’s consider a simplified example where a nomogram is used to predict the probability of a disease based on two factors: Age and Blood Pressure (BP).
    1. Age Scale: This scale might range from 20 to 80 years.
    2. BP Scale: This scale might range from 100 to 180 mmHg.
  • Nomogram plot
    Nomogram.png

Calibration Plot

Calibration plots are used to compare predicted probabilities from a model (like a logistic regression or a nomogram) with the actual observed outcomes. They help assess the accuracy of a prediction model.

Decision Curve Analysis (DCA)

Decision curve analysis evaluates the clinical usefulness of prediction models by comparing the net benefit of using the model to make decisions at various threshold probabilities.

Forest Plot

Forest plots are commonly used in meta-analysis to display the estimated effects from multiple studies.

Logistic Regression Curve

In binary logistic regression, the logistic curve (or S-curve) is used to model the probability of an event occurring based on a linear combination of predictor variables.

Score Plot (from Principal Component Analysis)

Partial Dependence Plot (PDP)

  • PDPs show the relationship between a predictor variable and the predicted outcome while accounting for the average effect of other predictors in the model.
  • CRAN, github
  • Interpretable Machine Learning by Christoph Molnar
  • Detailed breakdown:
    • How it works: For each value of the predictor variable of interest, the PDP is calculated by averaging the model’s predictions over the range of values for the other predictor variables. This isolates the effect of the predictor variable of interest from the effects of the other predictors.
    • Types of PDPs:
      • Univariate PDP: Shows the effect of a single predictor variable on the prediction.
      • Bivariate PDP: Shows the effect of two predictor variables together on the prediction.
  • Linear regression with two predictors X1 and X2
    # Load necessary libraries
    library(ggplot2)
    library(gridExtra)
    
    # Generate sample data
    set.seed(123)
    n <- 100
    X1 <- rnorm(n)
    X2 <- rnorm(n)
    Y <- 5 + 2*X1 + 3*X2 + rnorm(n)
    
    # Fit a linear regression model
    model <- lm(Y ~ X1 + X2)
    
    # Predict function for new data
    predict_model <- function(new_data) {
      predict(model, new_data)
    }
    
    # Partial Dependence Plot for X1
    pdp_X1 <- function(X1_values) {
      new_data <- data.frame(X1 = X1_values, X2 = mean(X2))
      predictions <- predict_model(new_data)
      data.frame(X1 = X1_values, Prediction = predictions)
    }
    
    # Partial Dependence Plot for X2
    pdp_X2 <- function(X2_values) {
      new_data <- data.frame(X1 = mean(X1), X2 = X2_values)
      predictions <- predict_model(new_data)
      data.frame(X2 = X2_values, Prediction = predictions)
    }
    
    # Generate values for PDPs
    X1_values <- seq(min(X1), max(X1), length.out = 100)
    X2_values <- seq(min(X2), max(X2), length.out = 100)
    
    # Create PDP data
    pdp_X1_data <- pdp_X1(X1_values)
    pdp_X2_data <- pdp_X2(X2_values)
    
    # Plot PDPs
    p1 <- ggplot(pdp_X1_data, aes(x = X1, y = Prediction)) +
      geom_line() +
      ggtitle("Partial Dependence Plot for X1") +
      xlab("X1") + ylab("Predicted Y")
    
    p2 <- ggplot(pdp_X2_data, aes(x = X2, y = Prediction)) +
      geom_line() +
      ggtitle("Partial Dependence Plot for X2") +
      xlab("X2") + ylab("Predicted Y")
    
    # Display plots
    grid.arrange(p1, p2, ncol = 2)
    
  • Cox regression.
    • Risk score [math]\displaystyle{ = \exp(\beta X) }[/math]. It is closely related to the hazard function h(t|X)=h0(t)exp(b*X).
    • If X=1, we obtained the HR. The hazard ratio (HR) represents the effect of a one-unit change in the predictor on the hazard.
    library(survival)
    library(ggplot2)
    
    set.seed(123)
    n <- 200
    X1 <- rnorm(n)
    X2 <- rnorm(n)
    time <- rexp(n, exp(0.5*X1 - 0.3*X2))
    status <- sample(0:1, n, replace = TRUE)
    
    # Fit the Cox model
    cox_model <- coxph(Surv(time, status) ~ X1 + X2)
    
    # Define the predictor range
    
    # Define the range of values for X1
    X1_values <- seq(min(X1), max(X1), length.out = 100)
    
    # Calculate the mean of X2
    X2_mean <- mean(X2)
    
    # Function to compute the risk score
    compute_risk_score <- function(X1_values, model, X2_mean) {
      new_data <- data.frame(X1 = X1_values, X2 = X2_mean)
      risk_score <- exp(predict(model, newdata = new_data, type = "lp")) # default
      # OR
      # risk_score <- predict(model, newdata = new_data, type = "risk") # risk score
      data.frame(X1 = X1_values, RiskScore = risk_score)
    }
    
    pdp_X1_data <- compute_risk_score(X1_values, cox_model, X2_mean)
    
    # The plot shows how the risk score changes with the predictor X1, holding X2 constant.
    # The baseline hazard function  h_0(t)  is not included in the PDP, as we are focusing 
    #   on the relative effects of predictors.
    # Plot PDP for X1
    ggplot(pdp_X1_data, aes(x = X1, y = HazardRatio)) +
      geom_line() +
      ggtitle("Partial Dependence Plot for X1 in Cox Regression") +
      xlab("X1") +
      ylab("Risk score")
    

    Use survival probability instead of risk score.

    # Define a function to compute survival probabilities
    compute_survival_prob <- function(X1_values, model, X2_mean) {
      new_data <- data.frame(X1 = X1_values, X2 = X2_mean)
      risk_score <- exp(predict(model, newdata = new_data, type = "lp")) # default
      # OR
      # risk_score <- predict(model, newdata = new_data, type = "risk")
      survival_prob <- baseline_survival_prob ^ risk_score
      return(survival_prob)
    }
    
    # Approximate survival probability (assuming a fixed time t for illustration)
    # You would need to adjust this based on your actual survival analysis
    # For demonstration purposes, we assume baseline survival probability at time t
    baseline_survival_prob <- 0.9  # S0(t) 
    
    # Compute survival probabilities for the range of X1 values
    survival_probs <- compute_survival_prob(X1_values, cox_model, X2_mean)
    
    library(ggplot2)
    
    # Create a data frame for plotting
    pdp_data <- data.frame(X1 = X1_values, SurvivalProbability = survival_probs)
    
    # Plot the survival function vs. predictor
    ggplot(pdp_data, aes(x = X1, y = SurvivalProbability)) +
      geom_line() +
      ggtitle("Partial Dependence Plot: Survival Function vs Predictor") +
      xlab("Predictor (X1)") +
      ylab("Survival Probability")
    

Quantile regression

  • Quantile regression is a type of regression analysis in which quantiles of the dependent variable (unlike traditional linear regression, which models the mean of the dependent variable) are modeled as a function of independent variables. This allows for a better understanding of the distribution of the dependent variable, especially when the distribution is skewed or has outliers.
  • https://en.wikipedia.org/wiki/Quantile_regression
  • Basic Quantile Regression
  • QUANTILE REGRESSION (HOME MADE, PART 2)
    library(quantreg)
    set.seed(123)
    x <- rnorm(100)
    y <- x + rnorm(100, mean = 0, sd = 2)
    y[1:10] <- y[1:10] + 10 # first 10 are outliers
    
    # Fit a traditional linear regression model
    fit_lm <- lm(y ~ x)
    
    # Fit a quantile regression model for the 50th percentile
    fit_qr <- rq(y ~ x, tau = 0.5)
    
    fit_lm$coefficients
    # (Intercept)           x 
    #   0.7961233   0.8759269 
    fit_qr$coefficients
    # (Intercept)           x 
    #   0.0772395   1.0058387 
    
    plot(x, y)
    points(x[1:10], y[1:10], col='red', pch=16)
    abline(fit_lm)
    abline(fit_qr, col = 'blue')
    
  • Navigating Quantile Regression with R: A Comprehensive Guide

Isotonic regression

Piecewise linear regression

Support vector regression

  • An Introduction to Support Vector Regression (SVR).
    • The goal of SVR is to find a function that approximates the relationship between the input and output variables in the training data, with an acceptable amount of error. This is done by mapping the input data into a high-dimensional feature space using a kernel function, and then finding a linear regression function in that space that fits the data with a specified margin of error.
    • SVR has been proven to be an effective tool in real-value function estimation, and like SVM, it is characterized by the use of kernels, sparse solution, and VC control of the margin and the number of support vectors.
  • Awad in Springer

Model Misspecification

Robust regression

Example 1: data with outliers

Below is an example where we fit the data using linear regression, robust linear regression (Robust against outliers and deviations from normality), quantile regression (Estimates conditional quantiles of the response variable), Theil-sen regression (Computes the median of pairwise slopes between data points) and Local polynomial regression (non-linear relationships and adapts to local variations).

DataOutliers.png

Example 2: data with outliers

The raw data are 'recovered' from the page Dealing with Outliers Using Three Robust Linear Regression Models. In this case, Theil-sen regression performed better than the other methods.

DataOutliers2.png

Choose variables

Variable selection in linear regression models: Choosing the best subset is not always the best choice 2023

Stepwise selection of variables

Stepwise selection of variables in regression is Evil

GEE/generalized estimating equations

See Longitudinal data analysis.

Deming regression

Deming regression

Tweedie regression

Model selection, AIC and Tweedie regression

Causal inference

  • The intuition behind inverse probability weighting in causal inference*, Confounding in causal inference: what is it, and what to do about it?
    Outcome [math]\displaystyle{ \begin{align} Y = T*Y(1) + (1-T)*Y(0) \end{align} }[/math]
    Causal effect (unobserved) [math]\displaystyle{ \begin{align} \tau = E(Y(1) -Y(0)) \end{align} }[/math]
    where [math]\displaystyle{ E[Y(1)] }[/math] referred to the expected outcome in the hypothetical situation that everyone in the population was assigned to treatment, [math]\displaystyle{ E[Y|T=1] }[/math] refers to the expected outcome for all individuals in the population who are actually assigned to treatment... The key is that the value of [math]\displaystyle{ E[Y|T=1]−E[Y|T=0] }[/math] is only equal to the causal effect, [math]\displaystyle{ E[Y(1)−Y(0)] }[/math] if there are no confounders present.
    Inverse-probability weighting removes confounding by creating a “pseudo-population” in which the treatment is independent of the measured confounders... Add a larger weight to the individuals who are underrepresented in the sample and a lower weight to those who are over-represented... propensity score P(T=1|X), logistic regression, stabilized weights.
  • A Crash Course in Causality: Inferring Causal Effects from Observational Data (Coursera) which includes Inverse Probability of Treatment Weighting (IPTW). R packages used: tableone, ipw, sandwich, survey.

Seemingly unrelated regressions/SUR

  • Seemingly unrelated regressions from wikipedia
    • Advantages: The SUR model is useful when the error terms of the regression equations are correlated with each other. In this case, the ordinary least squares (OLS) estimator is inefficient and inconsistent. The SUR model can provide more efficient and consistent estimates of the regression coefficients
    • Disadvantages: One disadvantage of using the SUR model is that it requires the assumption that the error terms are correlated across equations. If this assumption is not met, then the SUR model may not provide more efficient estimates than estimating each equation separately1. Another disadvantage of using the SUR model is that it can be computationally intensive and may require more time to estimate than estimating each equation separately
  • Seemingly Unrelated Regression (SUR/SURE)
  • How can I perform seemingly unrelated regression in R?
  • spsur package
  • Equations for the simplest case:
    [math]\displaystyle{ \begin{align} y_1 &= b_1x_1 + b_2x_2 + u_1 \\ y_2 &= b_3x_1 + b_4x_2 + u_2 \end{align} }[/math]