Functional phenotyping of genomic variants using joint multiomic single-cell DNA-RNA sequencing.

Lindenhofer, Dominik; Yildiz, Umut; Jung, Haeyeon; Huber, Wolfgang; Steinmetz, Lars M; Fitzgerald, Donnacha; Dietrich, Sascha; Kueblbeck, Moritz; Noh, Kyung-Min; Marttinen, Mikael; Korosteleva, Anastasiia; Bauman, Julia R; Zaugg, Judith B; Hawkins, John Andrew; Stegle, Oliver

doi:10.1038/s41592-025-02805-0

Items
Marc 21

001			304284
005			20250907022518.0
024	7	_	\|a 10.1038/s41592-025-02805-0 \|2 doi
024	7	_	\|a pmid:40890552 \|2 pmid
024	7	_	\|a 1548-7091 \|2 ISSN
024	7	_	\|a 1548-7105 \|2 ISSN
024	7	_	\|a altmetric:180897925 \|2 altmetric
037	_	_	\|a DKFZ-2025-01824
041	_	_	\|a English
082	_	_	\|a 610
100	1	_	\|a Lindenhofer, Dominik \|0 0000-0001-8838-7163 \|b 0
245	_	_	\|a Functional phenotyping of genomic variants using joint multiomic single-cell DNA-RNA sequencing.
260	_	_	\|a London [u.a.] \|c 2025 \|b Nature Publishing Group
336	7	_	\|a article \|2 DRIVER
336	7	_	\|a Output Types/Journal article \|2 DataCite
336	7	_	\|a Journal Article \|b journal \|m journal \|0 PUB:(DE-HGF)16 \|s 1756819045_26699 \|2 PUB:(DE-HGF)
336	7	_	\|a ARTICLE \|2 BibTeX
336	7	_	\|a JOURNAL_ARTICLE \|2 ORCID
336	7	_	\|a Journal Article \|0 0 \|2 EndNote
500	_	_	\|a epub
520	_	_	\|a Genetic variants (both coding and noncoding) can impact gene function and expression, driving disease mechanisms such as cancer progression. The systematic study of endogenous genetic variants is hindered by inefficient precision editing tools, combined with technical limitations in confidently linking genotypes to gene expression at single-cell resolution. We developed single-cell DNA-RNA sequencing (SDR-seq) to simultaneously profile up to 480 genomic DNA loci and genes in thousands of single cells, enabling accurate determination of coding and noncoding variant zygosity alongside associated gene expression changes. Using SDR-seq, we associate coding and noncoding variants with distinct gene expression in human induced pluripotent stem cells. Furthermore, we demonstrate that in primary B cell lymphoma samples, cells with a higher mutational burden exhibit elevated B cell receptor signaling and tumorigenic gene expression. SDR-seq provides a powerful platform to dissect regulatory mechanisms encoded by genetic variants, advancing our understanding of gene expression regulation and its implications for disease.
536	_	_	\|a 312 - Funktionelle und strukturelle Genomforschung (POF4-312) \|0 G:(DE-HGF)POF4-312 \|c POF4-312 \|f POF IV \|x 0
588	_	_	\|a Dataset connected to CrossRef, PubMed, , Journals: inrepo02.dkfz.de
700	1	_	\|a Bauman, Julia R \|0 0000-0001-9488-529X \|b 1
700	1	_	\|a Hawkins, John Andrew \|0 P:(DE-He78)f2456bb521cb457d6fcc86d06cbaf81e \|b 2 \|u dkfz
700	1	_	\|a Fitzgerald, Donnacha \|0 0000-0003-4927-7484 \|b 3
700	1	_	\|a Yildiz, Umut \|b 4
700	1	_	\|a Jung, Haeyeon \|0 0009-0001-7231-4573 \|b 5
700	1	_	\|a Korosteleva, Anastasiia \|0 0000-0002-5326-9471 \|b 6
700	1	_	\|a Marttinen, Mikael \|0 0000-0001-5861-4601 \|b 7
700	1	_	\|a Kueblbeck, Moritz \|0 0000-0001-6178-7140 \|b 8
700	1	_	\|a Zaugg, Judith B \|0 0000-0001-8324-4040 \|b 9
700	1	_	\|a Noh, Kyung-Min \|0 0000-0002-0708-787X \|b 10
700	1	_	\|a Dietrich, Sascha \|b 11
700	1	_	\|a Huber, Wolfgang \|0 0000-0002-0474-2218 \|b 12
700	1	_	\|a Stegle, Oliver \|0 P:(DE-He78)9aabcfee1a1fc9202398a45a63f0b1e3 \|b 13 \|u dkfz
700	1	_	\|a Steinmetz, Lars M \|0 0000-0002-3962-2865 \|b 14
773	_	_	\|a 10.1038/s41592-025-02805-0 \|0 PERI:(DE-600)2163081-1 \|p nn \|t Nature methods \|v nn \|y 2025 \|x 1548-7091
909	C	O	\|o oai:inrepo02.dkfz.de:304284 \|p VDB
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 2 \|6 P:(DE-He78)f2456bb521cb457d6fcc86d06cbaf81e
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 13 \|6 P:(DE-He78)9aabcfee1a1fc9202398a45a63f0b1e3
913	1	_	\|a DE-HGF \|b Gesundheit \|l Krebsforschung \|1 G:(DE-HGF)POF4-310 \|0 G:(DE-HGF)POF4-312 \|3 G:(DE-HGF)POF4 \|2 G:(DE-HGF)POF4-300 \|4 G:(DE-HGF)POF \|v Funktionelle und strukturelle Genomforschung \|x 0
914	1	_	\|y 2025
915	_	_	\|a Nationallizenz \|0 StatID:(DE-HGF)0420 \|2 StatID \|d 2025-01-07 \|w ger
915	_	_	\|a DEAL Nature \|0 StatID:(DE-HGF)3003 \|2 StatID \|d 2025-01-07 \|w ger
915	_	_	\|a JCR \|0 StatID:(DE-HGF)0100 \|2 StatID \|b NAT METHODS : 2022 \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0200 \|2 StatID \|b SCOPUS \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0300 \|2 StatID \|b Medline \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0600 \|2 StatID \|b Ebsco Academic Search \|d 2025-01-07
915	_	_	\|a Peer Review \|0 StatID:(DE-HGF)0030 \|2 StatID \|b ASC \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0199 \|2 StatID \|b Clarivate Analytics Master Journal List \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)1050 \|2 StatID \|b BIOSIS Previews \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0160 \|2 StatID \|b Essential Science Indicators \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)1030 \|2 StatID \|b Current Contents - Life Sciences \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)1190 \|2 StatID \|b Biological Abstracts \|d 2025-01-07
915	_	_	\|a WoS \|0 StatID:(DE-HGF)0113 \|2 StatID \|b Science Citation Index Expanded \|d 2025-01-07
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0150 \|2 StatID \|b Web of Science Core Collection \|d 2025-01-07
915	_	_	\|a IF >= 40 \|0 StatID:(DE-HGF)9940 \|2 StatID \|b NAT METHODS : 2022 \|d 2025-01-07
920	1	_	\|0 I:(DE-He78)B260-20160331 \|k B260 \|l B260 Bioinformatik der Genomik und Systemgenetik \|x 0
980	_	_	\|a journal
980	_	_	\|a VDB
980	_	_	\|a I:(DE-He78)B260-20160331
980	_	_	\|a UNRESTRICTED

Library	Collection	CLSMajor	CLSMinor	Language	Author

Marc 21

guest :: login DKFZ
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help