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Recent insights into inherited bone marrow failure syndromes

机译:对遗传性骨髓衰竭综合征的最新见解

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Purpose of review: Inherited bone marrow failure syndromes (IBMFS) are a diverse set of genetic disorders characterized by the inability of the bone marrow to produce sufficient circulating blood cells. The purpose of this review is to highlight novel findings in recent years and their impact on the understanding of IBMFS. Recent findings: Mutations in over 80 different genes have been associated with the development of bone marrow failure (BMF). The products of the genes mutated in IBMFS frequently participate in housekeeping pathways, which are important for cell growth and division rather than being specific for hematopoiesis. The common theme of these pathways, when disturbed, is the activation of p53, leading to cell cycle arrest, senescence, and cell death. With continued improvement in therapy for IBMFS, late complications, such as development of malignancies, are seen more frequently. This highlights the importance of understanding the affected pathways and their roles in cancer development. Summary: The recent advancement of our understanding of IBMFS has come largely through the identification of the genetic lesions responsible for disease and the investigations of their pathways. Applied in clinical practice, these findings make it possible to unambiguously identify mutation carriers even before the development of BMF and exclude or confirm a suspected clinical diagnosis for many of the more common IBMFS. The further characterization of the pathways leading to IBMFS is likely to reveal novel targets for screening tests, prognostic biomarkers, and improved and specific therapeutics.
机译:审查目的:遗传性骨髓衰竭综合征(IBMFS)是多种遗传疾病,其特征是骨髓无法产生足够的循环血细胞。本文的目的是重点介绍近年来的新颖发现及其对IBMFS理解的影响。最新发现:超过80种不同基因的突变与骨髓衰竭(BMF)的发生有关。在IBMFS中突变的基因产物经常参与管家通路,这对细胞生长和分裂很重要,而不是对造血功能具有特异性。这些途径的共同主题是,当受到干扰时,其是p53的激活,导致细胞周期停滞,衰老和细胞死亡。随着IBMFS治疗方法的不断改进,晚期并发症(例如恶性肿瘤的发生)的发生率越来越高。这突出了了解受影响的途径及其在癌症发展中的作用的重要性。简介:我们对IBMFS的了解的最新进展主要来自于鉴定导致疾病的遗传性病变及其途径。在临床实践中应用这些发现使得甚至在BMF发生之前就可以明确鉴定突变携带者,并排除或确认许多更常见的IBMFS的可疑临床诊断。导致IBMFS的途径的进一步表征可能会揭示用于筛选测试,预后生物标志物以及经过改进的特定治疗方法的新靶标。

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