Author:
Borgal Lori,Quiniou Margaux,Wakefield James
Abstract
AbstractMisregulation of candidate stem cell marker ASPM, and itsDrosophilahomologue Asp, leads to either tumour formation or microcephaly, but the functional roles contributing to each are not understood. We reverse-engineered flies to express a version of Asp (AspLIE), predicted to have lost its ability to bind the phosphatase PP2A-B’. Although AspLIEflies were viable, they exhibited splayed neural stem cell spindle poles under stress, and development was substantially delayed. A tissue-level analysis of microcephaly and midgut abnormalities in Asp mutants with a compromised spindle assembly checkpoint (SAC) demonstrates tissue-specific vulnerability to mitotic defects.
Publisher
Cold Spring Harbor Laboratory