Mosaic-variegated aneuploidy syndrome mutation or haploinsufficiency in Cep57 impairs tumor suppression
Khaled Aziz, … , David J. Katzmann, Jan M. van Deursen
Khaled Aziz, … , David J. Katzmann, Jan M. van Deursen
Published July 23, 2018
Citation Information: J Clin Invest. 2018;128(8):3517-3534. https://doi.org/10.1172/JCI120316.
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Research Article Cell biology Oncology

Mosaic-variegated aneuploidy syndrome mutation or haploinsufficiency in Cep57 impairs tumor suppression

Abstract

A homozygous truncating frameshift mutation in CEP57 (CEP57T/T) has been identified in a subset of mosaic-variegated aneuploidy (MVA) patients; however, the physiological roles of the centrosome-associated protein CEP57 that contribute to disease are unknown. To investigate these, we have generated a mouse model mimicking this disease mutation. Cep57T/T mice died within 24 hours after birth with short, curly tails and severely impaired vertebral ossification. Osteoblasts in lumbosacral vertebrae of Cep57T/T mice were deficient for Fgf2, a Cep57 binding partner implicated in diverse biological processes, including bone formation. Furthermore, a broad spectrum of tissues of Cep57T/T mice had severe aneuploidy at birth, consistent with the MVA patient phenotype. Cep57T/T mouse embryonic fibroblasts and patient-derived skin fibroblasts failed to undergo centrosome maturation in G2 phase, causing premature centriole disjunction, centrosome amplification, aberrant spindle formation, and high rates of chromosome missegregation. Mice heterozygous for the truncating frameshift mutation or a Cep57-null allele were overtly indistinguishable from WT mice despite reduced Cep57 protein levels, yet prone to aneuploidization and cancer, with tumors lacking evidence for loss of heterozygosity. This study identifies Cep57 as a haploinsufficient tumor suppressor with biologically diverse roles in centrosome maturation and Fgf2-mediated bone formation.

Authors

Khaled Aziz, Cynthia J. Sieben, Karthik B. Jeganathan, Masakazu Hamada, Brian A. Davies, Raul O. Fierro Velasco, Nazneen Rahman, David J. Katzmann, Jan M. van Deursen

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Figure 4

Cep57 truncation impairs recruitment of binding partners.

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Cep57 truncation impairs recruitment of binding partners. (A) Schematic ...
(A) Schematic representation of PCM organization in interphase and mitotic WT cells. Thickness of rings correlates with the amount of PCM component. (B) Representative images from interphase and metaphase MEFs labeled for Cep152 and centrin 2. Quantification of Cep152 signal intensity is shown on the right. (C) Representative images from interphase and metaphase MEFs labeled for Cep63 and centrin 2. Quantification of Cep63 signal intensity is shown on the right. (D) Representative images from interphase and metaphase MEFs labeled for Cep192 and centrin 2. Quantification of Cep192 signal intensity is shown on the right. Data represent mean ± SEM. Statistical significance in BF was determined using 1-way ANOVA followed by Tukey’s multiple-comparisons test. *P < 0.05, **P < 0.01, ***P < 0.001. Scale bars: 5 μm.