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.
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机译:已在一组镶嵌杂色非整倍性(MVA)患者中鉴定出CEP57的纯合性截短移码突变(CEP57 T / T );然而,未知与疾病有关的与中心体相关的蛋白CEP57的生理作用。为了研究这些,我们已经生成了模仿这种疾病突变的小鼠模型。 Cep57 T / T 小鼠出生后24小时内死亡,尾巴短而卷曲,椎骨骨化严重受损。 Cep57 T / T 小鼠腰ac椎骨中的成骨细胞缺乏Fgf2,Fgf2是Cep57的结合伴侣,涉及多种生物学过程,包括骨骼形成。此外,Cep57 T / T 小鼠的广泛组织在出生时具有严重的非整倍性,与MVA患者的表型一致。 Cep57 T / T 小鼠胚胎成纤维细胞和患者来源的皮肤成纤维细胞未能在G2期经历中心体成熟,导致过早的中心粒分离,中心体扩增,异常的纺锤体形成和染色体错配的高发生率。尽管Cep57蛋白水平降低,但截短移码突变或Cep57-null等位基因的杂合子与WT小鼠却没有明显区别,但易于发生非整倍化和癌变,肿瘤缺乏杂合性丧失的证据。这项研究将Cep57鉴定为单倍体不足的肿瘤抑制因子,在中心体成熟和Fgf2介导的骨形成中具有生物学上多种多样的作用。
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