作者
Gökçen Eraslan,Eugene Drokhlyansky,Shankara Anand,Evgenij Fiškin,Ayshwarya Subramanian,Michal Slyper,Jiali Wang,Nicholas Van Wittenberghe,John M. Rouhana,Julia Waldman,Orr Ashenberg,Monkol Lek,Danielle Dionne,Thet Su Win,Michael S. Cuoco,Olena Kuksenko,Alexander M. Tsankov,Philip A. Branton,Jamie L. Marshall,Anna Greka,Gad Getz,Ayellet V. Segrè,François Aguet,Orit Rozenblatt–Rosen,Kristin Ardlie,Aviv Regev
摘要
Understanding gene function and regulation in homeostasis and disease requires knowledge of the cellular and tissue contexts in which genes are expressed. Here, we applied four single-nucleus RNA sequencing methods to eight diverse, archived, frozen tissue types from 16 donors and 25 samples, generating a cross-tissue atlas of 209,126 nuclei profiles, which we integrated across tissues, donors, and laboratory methods with a conditional variational autoencoder. Using the resulting cross-tissue atlas, we highlight shared and tissue-specific features of tissue-resident cell populations; identify cell types that might contribute to neuromuscular, metabolic, and immune components of monogenic diseases and the biological processes involved in their pathology; and determine cell types and gene modules that might underlie disease mechanisms for complex traits analyzed by genome-wide association studies.