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Distinct Brca1 Mutations Differentially Reduce Hematopoietic Stem Cell Function

机译:不同的Brca1突变差异减少造血干细胞功能。

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BRCA1 is a well-known DNA repair pathway component and a tissue-specific tumor suppressor. However, its role in hematopoiesis is uncertain. Here, we report that a cohort of patients heterozygous for BRCA1 mutations experienced more hematopoietic toxicity from chemotherapy than those with BRCA2 mutations. To test whether this reflects a requirement for BRCA1 in hematopoiesis, we generated mice with Brca1 mutations in hematopoietic cells. Mice homozygous for a null Brca1 mutation in the embryonic hematopoietic system (Vav1-iCre;Brca1^F^2^2^-^2^4^/^F^2^2^-^2^4) developed hematopoietic defects in early adulthood that included reduced hematopoietic stem cells (HSCs). Although mice homozygous for a huBRCA1 knockin allele (Brca1^B^R^C^A^1^/^B^R^C^A^1) were normal, mice with a mutant huBRCA1/5382insC allele and a null allele (Mx1-Cre;Brca1^F^2^2^-^2^4^/^5^3^8^2^i^n^s^C) had severe hematopoietic defects marked by a complete loss of hematopoietic stem and progenitor cells. Our data show that Brca1 is necessary for HSC maintenance and normal hematopoiesis and that distinct mutations lead to different degrees of hematopoietic dysfunction.
机译:BRCA1是众所周知的DNA修复途径成分和组织特异性肿瘤抑制物。但是,其在造血中的作用尚不确定。在这里,我们报告说,BRCA1突变杂合的患者队列比BRCA2突变的患者经历了更多的化疗造血毒性。为了测试这是否反映了造血过程中对BRCA1的需求,我们生成了在造血细胞中具有Brca1突变的小鼠。纯合子在胚胎造血系统中的无效Brca1突变的小鼠(Vav1-iCre; Brca1 ^ F ^ 2 ^ 2 ^-^ 2 ^ 4 ^ / ^ F ^ 2 ^ 2 ^-^ 2 ^ 4)在早期形成了造血缺陷。成年时期包括减少的造血干细胞(HSC)。尽管huBRCA1敲入等位基因(Brca1 ^ B ^ R ^ C ^ A ^ 1 ^ / ^ B ^ R ^ C ^ A ^ 1)纯合的小鼠是正常的,但具有突变huBRCA1 / 5382insC等位基因和无效等位基因(Mx1)的小鼠-Cre; Brca1 ^ F ^ 2 ^ 2 ^-^ 2 ^ 4 ^ / ^ 5 ^ 3 ^ 8 ^ 2 ^ i ^ n ^ s ^ C)具有严重的造血缺陷,其特征是造血干细胞和祖细胞完全丧失。我们的数据表明,Brca1对于维持HSC和正常造血是必不可少的,并且不同的突变导致不同程度的造血功能障碍。

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