1. A Toy Example

To give a first impression of how DiscreteFDR works, we consider an artificial toy example. A more realistic example involving pharmacovigilance data is given in Section 2.

Suppose we would like to compare two treatments in nine different populations. For each population we do this by evaluating the responders and non-responders for each treatment. This leads to categorical data which can be represented, for each population $i = 1, \ldots, 9$ in the following 2 $\times$ 2 table:

	Responders	Non-responders
Treatment 1	$x_{1i}$	$y_{1i}$	$n_{1i}$
Treatment 2	$x_{2i}$	$y_{2i}$	$n_{2i}$
Total	$x_{1i} + x_{2i}$	$y_{1i} + y_{2i}$	$n = n_{1i} + n_{2i}$

Denoting the responder probabilities for population $i$ by $\pi_{1i}$ and $\pi_{2i}$ we can test e.g.

\[H_{0i}: \pi_{1i} = \pi_{2i} \qquad \text{vs.} \qquad H_{1i}: \pi_{1i} \neq \pi_{2i}\]

by using Fisher’s (two-sided) exact test (see Lehmann and Romano (2006)), which is implemented in the R function fisher.test. Suppose the data in the nine populations are independent and we observe the following data frame df

library(knitr)
X1 <- c(4, 2, 2, 14, 6, 9, 4, 0, 1)
X2 <- c(0, 0, 1, 3, 2, 1, 2, 2, 2)
N1 <- rep(148, 9)
N2 <- rep(132, 9)
Y1 <- N1 - X1
Y2 <- N2 - X2
df <- data.frame(X1, Y1, X2, Y2)
kable(df, caption = "Toy Example")

Toy Example
X1	Y1	X2	Y2
4	144	0	132
2	146	0	132
2	146	1	131
14	134	3	129
6	142	2	130
9	139	1	131
4	144	2	130
0	148	2	130
1	147	2	130

In this data frame each of the 9 rows represents the data of an observed 2 $\times$ 2 table: e.g., the third row of the data corresponds to $x_{13} = 2, y_{13} = 146, x_{23} = 1, y_{23} = 131$. Even though in this example, the total number of tested hypotheses $m = 9$ is very small, for illustrative purposes we deal with the multiplicity problem here by controlling FDR at level $\alpha = 5\%$. The DBH step-down procedure can be applied directly to the data frame object df and perform Fisher’s exact test in-between. This yields an S3 object of class DiscreteFDR, for which we provide both print and summary methods:

library(DiscreteFDR)
DBH.sd.fast <- direct.discrete.BH(df, "fisher", direction = "sd")
print(DBH.sd.fast)

## 
##   Discrete Benjamini-Hochberg procedure (step-down) 
## 
## Data:  df 
## Number of tests = 9 
## Number of rejections = 2 at global FDR level 0.05 
## (Original BH rejections = 0)
## Largest rejected p value:  0.02126871

summary(DBH.sd.fast)

## 
##   Discrete Benjamini-Hochberg procedure (step-down) 
## 
## Data:  df 
## Number of tests = 9 
## Number of rejections = 2 at global FDR level 0.05 
## (Original BH rejections = 0)
## Largest rejected p value:  0.02126871 
## 
##   Index    P.value   Adjusted Rejected
## 1     4 0.01243145 0.03819796     TRUE
## 2     6 0.02126871 0.03819796     TRUE
## 3     1 0.12476691 0.25630985    FALSE
## 4     8 0.22135177 0.47895996    FALSE
## 5     5 0.28849298 0.51482782    FALSE
## 6     2 0.49984639 1.00000000    FALSE
## 7     9 0.60329543 1.00000000    FALSE
## 8     7 0.68723229 1.00000000    FALSE
## 9     3 1.00000000 1.00000000    FALSE

The output of the summary function contains the same output as the print method, but adds a table that lists the raw $p$-values, their adjusted counterparts and their respective rejection decisions. It is sorted by raw $p$-values in ascending order. Our summary method actually creates a summary.DiscreteFDR object, which includes all contents of an DiscreteFDR object plus the aforementioned table. This table can be accessed directly by the $Table command.

DBH.sd.fast.summary <- summary(DBH.sd.fast)
summary.table <- DBH.sd.fast.summary$Table
kable(summary.table, caption = "Summary table")

Summary table
Index	P.value	Adjusted	Rejected
4	0.0124314	0.0381980	TRUE
6	0.0212687	0.0381980	TRUE
1	0.1247669	0.2563098	FALSE
8	0.2213518	0.4789600	FALSE
5	0.2884930	0.5148278	FALSE
2	0.4998464	1.0000000	FALSE
9	0.6032954	1.0000000	FALSE
7	0.6872323	1.0000000	FALSE
3	1.0000000	1.0000000	FALSE

Thus we can reject two hypotheses at FDR-level $\alpha = 5\%$. Note, that our print method also gives the number of rejections of the usual (continuous) BH procedure. In order to compare its adjusted $p$-values with ours, we have to determine the raw $p$-values first. This would be possible by applying the fisher.test function to all nine 2 $\times$ 2 tables. Alternatively, we may use the more convenient function generate.pvalues, which is included in our package, for accessing the raw $p$-values. Since it only accept hypothesis test functions from the package DiscreteTests (either as a function object or a character string that can be abbreviated), we could also use such a function directly, e.g. fisher.test.pv. An even more simple way is to extract them from the DiscreteFDR object that we obtained before and contains the results:

# compute results of Fisher's exact test for each row of 'df'
fisher.p <- generate.pvalues(df, "fisher", list(alternative = "two.sided"))
# extract raw observed p-values
raw.pvalues <- fisher.p$get_pvalues()

# or
library(DiscreteTests)
fisher.p.2 <- fisher.test.pv(df, "two.sided")
raw.pvalues.2 <- fisher.p.2$get_pvalues()

# or:
raw.pvalues.3 <- DBH.sd.fast$Data$raw.pvalues

all(raw.pvalues == raw.pvalues.2) && all(raw.pvalues == raw.pvalues.3)

## [1] TRUE

p.adjust(raw.pvalues, method = "BH")

## [1] 0.37430072 0.74976959 1.00000000 0.09570921 0.51928737 0.09570921 0.77313633
## [8] 0.49804147 0.77313633

Applying the continuous BH procedure from the stats package in the last line of code, we find that we cannot reject any hypotheses at FDR-level $\alpha = 5\%$. Another approach of determining this is to compare the critical values of the discrete and continuous BH procedures. In the discrete case, we need the observed $p$-values and their distributions. Both were computed by our generate.pvalues function above. We can either extract them and pass them to the DBH function, or directly apply the function to the test results object itself:

# extract raw observed p-values
raw.pvalues <- fisher.p$get_pvalues()
# extract p-value support sets
pCDFlist <- fisher.p$get_pvalue_supports()

# use raw pvalues and list of supports:
DBH.sd.crit <- DBH(raw.pvalues, pCDFlist, 0.05, "sd", TRUE)
crit.vals.BH.disc <- DBH.sd.crit$Critical.values

# use test results object directly
DBH.sd.crit.2 <- DBH(fisher.p, 0.05, "sd", TRUE)
crit.vals.BH.disc.2 <- DBH.sd.crit.2$Critical.values

# compare
all(crit.vals.BH.disc == crit.vals.BH.disc.2)

## [1] TRUE

The latter way enables the use of a pipe:

df |>
  fisher.test.pv(alternative = "two.sided") |>
  DBH(0.05, "sd", TRUE) |>
  with(Critical.values)

## [1] 0.01243145 0.02832448 0.03109596 0.04839433 0.05014119 0.07657062 0.07657062
## [8] 0.10328523 0.10328523

Now, we can compare the critical values:

crit.vals.BH.cont <- 1:9 * 0.05/9
tab <- data.frame(raw.pvalues = sort(raw.pvalues), crit.vals.BH.disc, crit.vals.BH.cont)
kable(tab, caption = "Observed p-values and critical values")

Observed p-values and critical values
raw.pvalues	crit.vals.BH.disc	crit.vals.BH.cont
0.0124314	0.0124314	0.0055556
0.0212687	0.0283245	0.0111111
0.1247669	0.0310960	0.0166667
0.2213518	0.0483943	0.0222222
0.2884930	0.0501412	0.0277778
0.4998464	0.0765706	0.0333333
0.6032954	0.0765706	0.0388889
0.6872323	0.1032852	0.0444444
1.0000000	0.1032852	0.0500000

Obviously, the critical values of the discrete approach are considerably larger than those of the continuous method. As a result, the two smallest $p$-values are rejected by the discrete BH procedure, because they are smaller than or equal to the respective critical values. The continuous BH approach does not reject any hypothesis, because all its critical values are smaller than the observed $p$-values.

For illustration, our package includes a plot method for DiscreteFDR S3 class objects. It allows to define colors, line types and point characters separately for accepted and rejected $p$-values and for critical values (if present in the object).

plot(DBH.sd.crit, col = c("red", "blue", "green"), pch = c(4, 2, 19), lwd = 2, type.crit = 'o',
     legend = "topleft", cex = 1.3)

Now, it is visible which observed $p$-values are rejected. A comparison with the continuous BH procedure could be done as follows:

plot(DBH.sd.crit, col = c("red", "blue", "green"), pch = c(4, 2, 19), lwd = 2, type.crit = 'o',
     cex = 1.3, ylim = c(0, 0.25), main = "Comparison of discrete and continuous BH procedures")
points(crit.vals.BH.cont, pch = 19, cex = 1.3, lwd = 2)
legend("topright", c("Rejected", "Accepted", "Critical Values (disc.)", "Critical Values (cont.)"),
       col = c("red", "blue", "green", "black"), pch = c(4, 2, 19, 19), lwd = 2, lty = 0)

As this example illustrates, the discrete approach can potentially yield a large increase in power. The gain depends on the involved distribution functions and the raw $p$-values. To appreciate where this comes from, it is instructive to consider the distribution functions $F_1, \ldots, F_9$ of the $p$-values under the null in more detail. Take for instance the first 2 $\times$ 2 table:

	Responders	Non-responders
Treatment 1	4	144	148
Treatment 2	0	132	132
Total	4	276	280

Fisher’s exact test works by determining the probability of observing this (or a more ‘extreme’) table, given that the margins are fixed. So each $F_i$ is determined by the margins of table $i$. Since $x_{11} + x_{21} = 4$, the only potentially observable tables are given by $x_{11} = 0, \ldots, 4$. For each one of these 5 values a $p$-value can be determined using the hypergeometric distribution. Therefore, the $p$-value of any 2 $\times$ 2 table with margins given by the above table can take (at most) 5 distinct values, say $x_1, \ldots, x_5$. Combining these 5 values into a set, we obtain the support $\mathcal{A}_1 = \{x_1, \ldots, x_5\}$ of distribution $F_1$. Now we can continue in this vein for the remaining 2 $\times$ 2 tables to obtain the supports $\mathcal{A}_1, \ldots, \mathcal{A}_9$ for the distribution functions $F_1, \ldots, F_{9}$. The supports can be accessed via the $get_pvalue_supports() function of the results object, e.g.

# extract p-value support sets
pCDFlist <- fisher.p$get_pvalue_supports()
# extract 1st and 5th support set
pCDFlist[c(1,5)]

## [[1]]
## [1] 0.04820493 0.12476691 0.34598645 0.62477763 1.00000000
## 
## [[2]]
## [1] 0.002173856 0.007733719 0.028324482 0.069964309 0.154043258 0.288492981
## [7] 0.481808361 0.726262402 1.000000000

Here, this returns $\mathcal{A}_1$ and $\mathcal{A}_5$. Panel (a) in the following figure shows a graph of the distribution functions $F_1, \ldots, F_9$. Each $F_i$ is a step-function with $F_i(0) = 0$, the jumps occurring only on the support $\mathcal{A}_i$ and $F_i(x) = x$ only for $x \in \mathcal{A}_i$. In particular, all distributions are stochastically larger than the uniform distribution (i.e., $F_i(x) \le x$), but in a heterogeneous manner. This heterogeneity can be exploited e.g., by transforming the raw $p$-values from the exact Fisher’s test using the function \[\displaystyle \xi_{\text{SD}}(x) = \sum_{i = 1}^{9} \frac{F_i(x)}{1 - F_i(x)}.\] Panel (b) of the following plot shows that $\xi_{\text{SD}}$ is a step function. Its jumps occur on the joint support $\mathcal{A}= \mathcal{A}_1 \cup \ldots \cup \mathcal{A}_9$. Panel (b) also shows that $\displaystyle \xi_{\text{SD}}(x) \ll x$, at least for small values of $x$. It turns out that the critical values of our new DBH step-down procedure are essentially given by inverting $\xi_{\text{SD}}$ at the critical values of the [BH] procedure $1 \cdot \alpha / 9, 2 \cdot \alpha / 9, \ldots, \alpha$, so that these values are considerably larger than the [BH] critical values. This is illustrated in panel (c) along with the ordered $p$~values. In particular, all asterisks are located above the green [BH] dots, therefore this procedure can not reject any hypothesis. In contrast, the two smallest $p$~values are located below red DBH step-down dots, so that this procedure rejects two hypotheses as we had already seen earlier.

stepf <- lapply(pCDFlist, function(x) stepfun(x, c(0, x)))
par(mfcol = c(1, 3), mai = c(1, 0.5, 0.3, 0.1))
plot(stepf[[1]], xlim = c(0, 1), ylim = c(0, 1), do.points = FALSE, lwd = 1, lty = 1, ylab = "F(x)", 
     main = "(a)")
for(i in (2:9)){
  plot(stepf[[i]], add = TRUE, do.points = FALSE, lwd = 1, col = i)
}
segments(0, 0, 1, 1, col = "grey", lty = 2)

#   Plot xi
support <- sort(unique(unlist(pCDFlist)))
components <- lapply(stepf, function(s){s(support) / (1 - s(support))}) 
xi.values <- 1/9 * Reduce('+', components)
xi <- stepfun(support, c(0, xi.values))
plot(xi, xlim = c(0, 0.10), ylim = c(0, 0.10), do.points = FALSE, ylab = expression(xi), main = "(b)")
segments(0, 0, 0.1, 0.1, col = "grey", lty = 2)

#   Plot discrete critical values as well a BH constants and raw p-values
DBH.sd <- DBH(fisher.p, direction = "sd", ret.crit.consts = TRUE)
plot(DBH.sd, col = c("black", "black", "red"), pch = c(4, 4, 19), type.crit = 'p', ylim = c(0, 0.15),
     cex = 1.3, main = "(c)", ylab = "Critical Values")
points(1:9, 0.05 * (1:9) / 9, col = "green", pch = 19, cex = 1.3)

mtext("Figure 1", 1, outer = TRUE, line = -2)

Panel (a) depicts the distribution functions $F_1, \ldots, F_9$ in various colors, (b) is a graph of the transformation $\xi_{\text{SD}}$. The uniform distribution function is shown in light gray in (a) and (b). Panel (c) shows the [BH] critical values (green dots), the DBH step-down critical values (red dots) and the sorted raw $p$-values (asterisks).

	Responders	Non-responders
Treatment 1	\(x_{1i}\)	\(y_{1i}\)	\(n_{1i}\)
Treatment 2	\(x_{2i}\)	\(y_{2i}\)	\(n_{2i}\)
Total	\(x_{1i} + x_{2i}\)	\(y_{1i} + y_{2i}\)	\(n = n_{1i} + n_{2i}\)

X1	Y1	X2	Y2
4	144	0	132
2	146	0	132
2	146	1	131
14	134	3	129
6	142	2	130
9	139	1	131
4	144	2	130
0	148	2	130
1	147	2	130

X1	Y1	X2	Y2
4	144	0	132
2	146	0	132
2	146	1	131
14	134	3	129
6	142	2	130
9	139	1	131
4	144	2	130
0	148	2	130
1	147	2	130

X1	Y1	X2	Y2
4	144	0	132
2	146	0	132
2	146	1	131
14	134	3	129
6	142	2	130
9	139	1	131
4	144	2	130
0	148	2	130
1	147	2	130