生物
移码突变
表型
肾上腺功能不全
突变
自然杀伤细胞
细胞生长
细胞
基因
免疫学
遗传学
细胞毒性T细胞
体外
作者
Laure Gineau,Céline Cognet,Nihan Kara,Francis P. Lach,Jean Dunne,Uma Veturi,Capucine Pïcard,Céline Trouillet,Céline Eidenschenk,Saïd Aoufouchi,Alexandre Alcaïs,Owen Smith,Frédéric Geissmann,Conleth Feighery,Laurent Abel,Agata Smogorzewska,Bruce Stillman,Éric Vivier,Jean‐Laurent Casanova,Emmanuelle Jouanguy
摘要
Natural killer (NK) cells are circulating cytotoxic lymphocytes that exert potent and nonredundant antiviral activity and antitumoral activity in the mouse; however, their function in host defense in humans remains unclear. Here, we investigated 6 related patients with autosomal recessive growth retardation, adrenal insufficiency, and a selective NK cell deficiency characterized by a lack of the CD56dim NK subset. Using linkage analysis and fine mapping, we identified the disease-causing gene, MCM4, which encodes a component of the MCM2-7 helicase complex required for DNA replication. A splice-site mutation in the patients produced a frameshift, but the mutation was hypomorphic due to the creation of two new translation initiation methionine codons downstream of the premature termination codon. The patients’ fibroblasts exhibited genomic instability, which was rescued by expression of WT MCM4. These data indicate that the patients’ growth retardation and adrenal insufficiency likely reflect the ubiquitous but heterogeneous impact of the MCM4 mutation in various tissues. In addition, the specific loss of the NK CD56dim subset in patients was associated with a lower rate of NK CD56bright cell proliferation, and the maturation of NK CD56bright cells toward an NK CD56dim phenotype was tightly dependent on MCM4-dependent cell division. Thus, partial MCM4 deficiency results in a genetic syndrome of growth retardation with adrenal insufficiency and selective NK deficiency.
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