Precise modulation of transcription factor levels identifies features underlying dosage sensitivity

Author:

Naqvi SahinORCID,Kim Seungsoo,Hoskens Hanne,Matthews Harold S.,Spritz Richard A.ORCID,Klein Ophir D.ORCID,Hallgrímsson BenediktORCID,Swigut Tomek,Claes PeterORCID,Pritchard Jonathan K.ORCID,Wysocka JoannaORCID

Abstract

AbstractTranscriptional regulation exhibits extensive robustness, but human genetics indicates sensitivity to transcription factor (TF) dosage. Reconciling such observations requires quantitative studies of TF dosage effects at trait-relevant ranges, largely lacking so far. TFs play central roles in both normal-range and disease-associated variation in craniofacial morphology; we therefore developed an approach to precisely modulate TF levels in human facial progenitor cells and applied it to SOX9, a TF associated with craniofacial variation and disease (Pierre Robin sequence (PRS)). Most SOX9-dependent regulatory elements (REs) are buffered against small decreases in SOX9 dosage, but REs directly and primarily regulated by SOX9 show heightened sensitivity to SOX9 dosage; these RE responses partially predict gene expression responses. Sensitive REs and genes preferentially affect functional chondrogenesis and PRS-like craniofacial shape variation. We propose that such REs and genes underlie the sensitivity of specific phenotypes to TF dosage, while buffering of other genes leads to robust, nonlinear dosage-to-phenotype relationships.

Funder

Howard Hughes Medical Institute

JW was supported by a Lorry Lokey endowed professorship and a Stinehart Reed award

Helen Hay Whitney Foundation

Damon Runyon Cancer Research Foundation

U.S. Department of Health & Human Services | National Institutes of Health

KU Leuven

The Research Program of the Research Foundation - Flanders (Belgium)

Publisher

Springer Science and Business Media LLC

Subject

Genetics

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