Reference: Yin H, et al. (2025) Inducible chromosomal rearrangement reveals nonlinear polygenic dosage effects in driving aneuploid yeast traits. Nat Commun 16(1):10884

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Abstract


Aneuploidy induces chromosomal scale alterations in gene dosage, impacting organismal proliferation yet serving as a driver for adaptive evolution. The complexity of gene dosage effects makes it challenging to elucidate the causal genetic basis of aneuploid consequence. Here, using loss-of-function screening with Synthetic Chromosome Rearrangement and Modification by LoxP-mediated Evolution (SCRaMbLE) in synthetic aneuploid yeast, in conjunction with gain-of-function testing in euploid yeast, we established a sufficient and necessary framework and discovered cases of nonlinear polygenic dosage effects in driving aneuploid phenotypes. We identified an emergent effect resulting from copy number alterations in a locus of five genes, which enhance trehalose biosynthesis and confer heat tolerance in aneuploid yeast with additional chromosome III. Additionally, a gene dosage-dependent antagonistic epistasis effect of two genes YCL039W and YCL037C determines rapamycin resistance in aneuploid yeast by regulating the Ras signaling pathway. Moreover, several cases of sufficiency-necessity asymmetries were found for other aneuploid traits. Together, our findings provide direct evidence of various dosage-dependent nonlinear polygenic interactions in shaping aneuploid phenotypes and advance understanding of the genetic basis of cellular adaptive evolution.

Reference Type
Journal Article
Authors
Yin H, Guo Z, Zhou C, Ma L, Wu Y, Yuan YJ
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