| Literature DB >> 27996937 |
Andres M Lebensohn1,2, Ramin Dubey1,2, Leif R Neitzel3, Ofelia Tacchelly-Benites4, Eungi Yang4, Caleb D Marceau5, Eric M Davis6, Bhaven B Patel1,2, Zahra Bahrami-Nejad7, Kyle J Travaglini1, Yashi Ahmed4, Ethan Lee3, Jan E Carette5, Rajat Rohatgi1,2.
Abstract
The comprehensive understanding of cellular signaling pathways remains a challenge due to multiple layers of regulation that may become evident only when the pathway is probed at different levels or critical nodes are eliminated. To discover regulatory mechanisms in canonical WNT signaling, we conducted a systematic forward genetic analysis through reporter-based screens in haploid human cells. Comparison of screens for negative, attenuating and positive regulators of WNT signaling, mediators of R-spondin-dependent signaling and suppressors of constitutive signaling induced by loss of the tumor suppressor adenomatous polyposis coli or casein kinase 1α uncovered new regulatory features at most levels of the pathway. These include a requirement for the transcription factor AP-4, a role for the DAX domain of AXIN2 in controlling β-catenin transcriptional activity, a contribution of glycophosphatidylinositol anchor biosynthesis and glypicans to R-spondin-potentiated WNT signaling, and two different mechanisms that regulate signaling when distinct components of the β-catenin destruction complex are lost. The conceptual and methodological framework we describe should enable the comprehensive understanding of other signaling systems.Entities:
Keywords: APC; AXIN; CSNK1A1; GPC4; GPI; HAP1; HUWE1; RSPO; SERBP1; TFAP4; WNT signaling; computational biology; developmental biology; forward genetics; genetic screen; glypican; haploid cells; haploid screen; human; stem cells; suppressor screen; systems biology
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Year: 2016 PMID: 27996937 PMCID: PMC5257257 DOI: 10.7554/eLife.21459
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140