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在果蝇眼中,棘突异构体参与不同的极化事件。

Prickle isoform participation in distinct polarization events in the Drosophila eye.

机构信息

Department of Pathology, Stanford University School of Medicine, Stanford, CA, United States of America.

出版信息

PLoS One. 2022 Feb 11;17(2):e0262328. doi: 10.1371/journal.pone.0262328. eCollection 2022.

Abstract

Planar cell polarity (PCP) signaling regulates several polarization events during development of ommatidia in the Drosophila eye, including directing chirality by polarizing a cell fate choice and determining the direction and extent of ommatidial rotation. The pksple isoform of the PCP protein Prickle is known to participate in the R3/R4 cell fate decision, but the control of other polarization events and the potential contributions of the three Pk isoforms have not been clarified. Here, by characterizing expression and subcellular localization of individual isoforms together with re-analyzing isoform specific phenotypes, we show that the R3/R4 fate decision, its coordination with rotation direction, and completion of rotation to a final ±90° rotation angle are separable polarization decisions with distinct Pk isoform requirements and contributions. Both pksple and pkpk can enforce robust R3/R4 fate decisions, but only pksple can correctly orient them along the dorsal-ventral axis. In contrast, pksple and pkpk can fully and interchangeably sustain coordination of rotation direction and rotation to completion. We propose that expression dynamics and competitive interactions determine isoform participation in these processes. We propose that the selective requirement for pksple to orient the R3/R4 decision and their interchangeability for coordination and completion of rotation reflects their previously described differential interaction with the Fat/Dachsous system which is known to be required for orientation of R3/R4 decisions but not for coordination or completion of rotation.

摘要

平面细胞极性 (PCP) 信号通路在果蝇眼睛的小眼发育过程中调节了几个极化事件,包括通过极化细胞命运选择来指导手性,以及确定小眼旋转的方向和程度。已知 PCP 蛋白 Prickle 的 pksple 同工型参与 R3/R4 细胞命运决定,但其他极化事件的控制以及三种 Pk 同工型的潜在贡献尚未阐明。在这里,我们通过描述单个同工型的表达和亚细胞定位以及重新分析同工型特异性表型,表明 R3/R4 命运决定、其与旋转方向的协调以及最终旋转到±90°旋转角度的完成是可分离的极化决定,具有不同的 Pk 同工型要求和贡献。pksple 和 pkpk 都可以强制进行强大的 R3/R4 命运决定,但只有 pksple 可以沿着背腹轴正确地对其进行定位。相比之下,pksple 和 pkpk 可以完全且可互换地维持旋转方向和完成旋转的协调。我们提出表达动态和竞争相互作用决定同工型在这些过程中的参与。我们提出,pksple 选择性地参与定位 R3/R4 决定以及它们在协调和完成旋转中的可互换性反映了它们与 Fat/Dachsous 系统的先前描述的差异相互作用,已知该系统对于 R3/R4 决定的定向是必需的,但对于协调或完成旋转不是必需的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26f8/8836327/baf7d8a8b1f6/pone.0262328.g001.jpg

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