CAML loss causes anaphase failure and chromosome missegregation

Calcium modulating cyclophilin ligand (CAML) is a ubiquitously expressed cytoplasmic protein that is implicated in the EGFR and LCK signaling pathways and required for early embryonic and thymocyte development. To further define the critical biological functions of CAML at the cellular level, we gen...

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Published inCell cycle (Georgetown, Tex.) Vol. 8; no. 6; pp. 940 - 949
Main Authors Liu, Yu, Malureanu, Liviu, Jeganathan, Karthik B., Tran, David Dinh, Lindquist, Lonn D., van Deursen, Jan M., Bram, Richard J.
Format Journal Article
LanguageEnglish
Published United States Taylor & Francis 15.03.2009
Subjects
Adaptor Proteins, Signal Transducing - genetics
Adaptor Proteins, Signal Transducing - metabolism
Anaphase - genetics
Animals
Binding
Biology
Bioscience
Calcium
Cancer
Cell
Cells, Cultured
Chromosomal Instability - genetics
Chromosome Segregation - genetics
Cycle
Fibroblasts - cytology
Fibroblasts - metabolism
Gene Knockout Techniques
Landes
Mice
Organogenesis
Proteins
Spindle Apparatus - metabolism
Spindle Apparatus - ultrastructure
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Summary:Calcium modulating cyclophilin ligand (CAML) is a ubiquitously expressed cytoplasmic protein that is implicated in the EGFR and LCK signaling pathways and required for early embryonic and thymocyte development. To further define the critical biological functions of CAML at the cellular level, we generated CAML-deleted mouse embryonic fibroblasts (MEFs) using an in vitro Cre-loxP mediated conditional knockout system. We found that CAML-/- MEFs have severely impaired proliferation and a strong reduction of normal anaphases. The primary mitotic defect of CAML-/- MEFs is that duplicated chromosomes fail to segregate in anaphase, resulting in nuclear bisection by the cleavage furrow as cells decondense their DNA and exit mitosis, highly reminiscent of the "cut" phenotype in fission yeast. This phenotype is due to spindle dysfunction rather than inability to resolve physical connections between sister chromatids. Furthermore, CAML-/- MEFs display defects often seen in cells with mitotic checkpoint gene deficiencies, including lagging and misaligned chromosomes and chromatin bridges. Consistent with this, we found that CAML-/- MEFs have a modestly weakened spindle assembly checkpoint (SAC) and increased aneuploidy. Thus, our data identify CAML as a novel chromosomal instability gene and suggest that CAML protein acts as a key regulator of mitotic spindle function and a modulator of SAC maintenance.
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ISSN:1538-4101
1551-4005
DOI:10.4161/cc.8.6.7948