Journal article
Image-based, pooled phenotyping reveals multidimensional, disease-specific variant effects
S Pendyala, K Partington, N Bradley, AE McEwen, G Straub, HJ Kim, S Fayer, DL Holmes, KA Sitko, RK Garge, ZR Wang, MK Wheelock, AJ Vandi, RL Powell, CE Friedman, E McDermot, N Kishore, FP Roth, AF Rubin, KC Yang Show all
Cell | Published : 2026
Abstract
Genetic variants produce complex phenotypic effects that confound current assays and predictive models. We developed variant in situ sequencing (VIS-seq), a pooled, image-based method measuring variant effects on molecular and cellular phenotypes in diverse cell types. Applying VIS-seq to ∼3,000 LMNA and PTEN variants yielded high-dimensional morphological profiles capturing changes in protein abundance, localization, activity, and cell architecture. VIS-seq identified a subset of linker-subdomain LMNA variants that increase nuclear circularity, in contrast to aggregating or low-abundance rod-subdomain variants that decrease circularity. VIS-seq also identified autism-associated PTEN variant..
View full abstractGrants
Awarded by NIGMS NIH HHS
Awarded by NHGRI NIH HHS