From 9fdfcc6da5fa7e9b54a7d207903b55d82856fe52 Mon Sep 17 00:00:00 2001
From: Federico Marini <marinif@uni-mainz.de>
Date: Thu, 21 Jul 2022 15:42:15 +0200
Subject: [PATCH] Update diffUTR.Rmd

---
 vignettes/diffUTR.Rmd | 2 +-
 1 file changed, 1 insertion(+), 1 deletion(-)

diff --git a/vignettes/diffUTR.Rmd b/vignettes/diffUTR.Rmd
index 5fda057..9630f41 100644
--- a/vignettes/diffUTR.Rmd
+++ b/vignettes/diffUTR.Rmd
@@ -39,7 +39,7 @@ and produce highly similar outputs, so that they can all be used with the same
 downstream plotting functions (Figure 1A).
 
 Based on various benchmarks (e.g. 
-[Sonenson et al. 2016](https://genomebiology.biomedcentral.com/articles/10.1186/s13059-015-0862-3);
+[Soneson et al. 2016](https://genomebiology.biomedcentral.com/articles/10.1186/s13059-015-0862-3);
 see also [our paper](https://doi.org/10.1186/s12859-021-04114-7)), 
 `r BiocStyle::Biocpkg("DEXSeq")` is the most accurate of the three methods, 
 and should therefore be the method of choice. It is however very slow and does