Clinical implementation of single-cell RNA sequencing using liver fine needle aspirate tissue sampling and centralized processing captures compartment specific immuno-diversity

Author:

Genshaft Alex S.,Subudhi SonuORCID,Keo Arlin,Vasquez Juan D. Sanchez,Conceição-Neto Nádia,Mahamed Deeqa,Boeijen Lauke L.,Alatrakchi Nadia,Oetheimer Chris,Vilme Mike,Drake Riley,Fleming Ira,Tran Nancy,Tzouanas Constantine,Joseph-Chazan Jasmin,Villanueva Martin Arreola,van de Werken Harmen J. G.ORCID,van Oord Gertine W.,Groothuismink Zwier M.A.,Beudeker Boris J.,Osmani Zgjim,Nkongolo Shirin,Mehrotra Aman,Feld Jordan,Chung Raymond T.,de Knegt Robert J.,Janssen Harry L. A.,Aerssens Jeroen,Bollekens Jacques,Hacohen Nir,Lauer Georg M.,Boonstra Andre,Shalek Alex K.,Gehring Adam

Abstract

AbstractBlood samples are frequently collected in human studies of the immune system but poorly represent tissue-resident immunity. Understanding the immunopathogenesis of tissue-restricted diseases, such as chronic hepatitis B, necessitates direct investigation of local immune responses. We developed a workflow that enables frequent, minimally invasive collection of liver fine-needle aspirates in multi-site international studies and centralized single-cell RNA sequencing data generation using the Seq-Well S3 picowell-based technology. All immunological cell types were captured, including liver macrophages, and showed distinct compartmentalization and transcriptional profiles, providing a systematic assessment of the capabilities and limitations of peripheral blood samples when investigating tissue-restricted diseases. The ability to electively sample the liver of chronic viral hepatitis patients and generate high-resolution data will enable multi-site clinical studies to power fundamental and therapeutic discovery.

Publisher

Cold Spring Harbor Laboratory

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