Abnormal chondrocyte development in a zebrafish model of cblC syndrome restored by an MMACHC cobalamin binding mutant

IF 2.2 3区生物学 Q4 CELL BIOLOGY Differentiation Pub Date : 2023-05-01 DOI:10.1016/j.diff.2023.04.003

David Paz , Briana E. Pinales , Barbara S. Castellanos , Isaiah Perez , Claudia B. Gil , Lourdes Jimenez Madrigal , Nayeli G. Reyes-Nava , Victoria L. Castro , Jennifer L. Sloan , Anita M. Quintana

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引用次数: 1

Abstract

Variants in the MMACHC gene cause combined methylmalonic acidemia and homocystinuria cblC type, the most common inborn error of intracellular cobalamin (vitamin B12) metabolism. cblC is associated with neurodevelopmental, hematological, ocular, and biochemical abnormalities. In a subset of patients, mild craniofacial dysmorphia has also been described. Mouse models of Mmachc deletion are embryonic lethal but cause severe craniofacial phenotypes such as facial clefts. MMACHC encodes an enzyme required for cobalamin processing and variants in this gene result in the accumulation of two metabolites: methylmalonic acid (MMA) and homocysteine (HC). Interestingly, other inborn errors of cobalamin metabolism, such as cblX syndrome, are associated with mild facial phenotypes. However, the presence and severity of MMA and HC accumulation in cblX syndrome is not consistent with the presence or absence of facial phenotypes. Thus, the mechanisms by which mutations in MMACHC cause craniofacial defects are yet to be completely elucidated. Here we have characterized the craniofacial phenotypes in a zebrafish model of cblC (hg13) and performed restoration experiments with either a wildtype or a cobalamin binding deficient MMACHC protein. Homozygous mutants did not display gross morphological defects in facial development but did have abnormal chondrocyte nuclear organization and an increase in the average number of neighboring cell contacts, both phenotypes were fully penetrant. Abnormal chondrocyte nuclear organization was not associated with defects in the localization of neural crest specific markers, sox10 (RFP transgene) or barx1. Both nuclear angles and the number of neighboring cell contacts were fully restored by wildtype MMACHC and a cobalamin binding deficient variant of the MMACHC protein. Collectively, these data suggest that mutation of MMACHC causes mild to moderate craniofacial phenotypes that are independent of cobalamin binding.

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MMACHC钴胺结合突变体恢复cblC综合征斑马鱼模型的异常软骨细胞发育

MMAACHC基因变异导致甲基丙二酸血症和高胱氨酸尿症cblC型，这是细胞内钴胺素（维生素B12）代谢最常见的先天性错误。cblC与神经发育、血液学、眼部和生化异常有关。在一部分患者中，还描述了轻度颅面畸形。Mmachc缺失的小鼠模型是胚胎致死的，但会导致严重的颅面表型，如面部裂隙。MMAACHC编码钴胺素加工所需的酶，该基因的变体导致两种代谢产物的积累：甲基丙二酸（MMA）和同型半胱氨酸（HC）。有趣的是，钴胺素代谢的其他先天性错误，如cblX综合征，与轻度面部表型有关。然而，cblX综合征中MMA和HC积聚的存在和严重程度与面部表型的存在或不存在并不一致。因此，MMAACHC突变导致颅面缺损的机制尚待完全阐明。在这里，我们对cblC（hg13）斑马鱼模型中的颅面表型进行了表征，并用野生型或钴胺素结合缺陷型MMAACHC蛋白进行了修复实验。纯合突变体在面部发育中没有表现出明显的形态学缺陷，但确实有异常的软骨细胞核组织和相邻细胞接触的平均数量增加，这两种表型都是完全渗透的。软骨细胞核组织异常与神经嵴特异性标记物sox10（RFP转基因）或barx1的定位缺陷无关。野生型MMAACHC和MMAACHC蛋白的钴胺素结合缺陷变体完全恢复了细胞核角度和相邻细胞接触的数量。总之，这些数据表明，MMAACHC的突变导致轻度至中度颅面表型，这些表型独立于钴胺素结合。

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来源期刊

Differentiation 生物-发育生物学

CiteScore

4.10

自引率

3.40%

发文量

审稿时长

51 days

期刊介绍： Differentiation is a multidisciplinary journal dealing with topics relating to cell differentiation, development, cellular structure and function, and cancer. Differentiation of eukaryotes at the molecular level and the use of transgenic and targeted mutagenesis approaches to problems of differentiation are of particular interest to the journal. The journal will publish full-length articles containing original work in any of these areas. We will also publish reviews and commentaries on topics of current interest. The principal subject areas the journal covers are: • embryonic patterning and organogenesis • human development and congenital malformation • mechanisms of cell lineage commitment • tissue homeostasis and oncogenic transformation • establishment of cellular polarity • stem cell differentiation • cell reprogramming mechanisms • stability of the differentiated state • cell and tissue interactions in vivo and in vitro • signal transduction pathways in development and differentiation • carcinogenesis and cancer • mechanisms involved in cell growth and division especially relating to cancer • differentiation in regeneration and ageing • therapeutic applications of differentiation processes.

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