AI Article Synopsis

  • Dynein is an important motor protein that helps organize cells, but its production and function are not well understood.
  • Researchers conducted a CRISPR screen on human cells to identify genes that affect dynein's ability to transport cellular structures, leading to the discovery of 195 relevant gene targets.
  • One notable finding was that the RNA-binding protein SUGP1 enhances dynein function by supporting the activity of another protein, LIS1, which plays a role in cargo movement within cells.

Article Abstract

The microtubule motor dynein plays a key role in cellular organization. However, little is known about how dynein's biosynthesis, assembly, and functional diversity are orchestrated. To address this issue, we have conducted an arrayed CRISPR loss-of-function screen in human cells using the distribution of dynein-tethered peroxisomes and early endosomes as readouts. From a genome-wide gRNA library, 195 validated hits were recovered and parsed into those impacting multiple dynein cargoes and those whose effects are restricted to a subset of cargoes. Clustering of high-dimensional phenotypic fingerprints revealed co-functional proteins involved in many cellular processes, including several candidate novel regulators of core dynein functions. Further analysis of one of these factors, the RNA-binding protein SUGP1, indicates that it promotes cargo trafficking by sustaining functional expression of the dynein activator LIS1. Our data represent a rich source of new hypotheses for investigating microtubule-based transport, as well as several other aspects of cellular organization captured by our high-content imaging.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10916854PMC
http://dx.doi.org/10.1083/jcb.202306048DOI Listing

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