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恶性造血细胞中近单倍体的起源。

Origin of near-haploidy in malignant hematopoietic cells.

作者信息

Verma R S, Macera M J, Silver R T, Coleman M

机构信息

Division of Genetics, Long Island College Hospital, Brooklyn, NY 10021.

出版信息

Leuk Res. 1988;12(11-12):941-50. doi: 10.1016/0145-2126(88)90022-7.

Abstract

Hyperdiploidy is common in neoplastic diseases but severe hypodiploidy or near-haploidy is extremely rare. Acute lymphocytic leukemia (ALL) and blast phase of chronic myelocytic leukemia (BC/CML) are the two most common leukemias where metaphases with as low as 23 chromosomes have been reported. Recent studies have indicated that during the course of malignant development, cells undergo numerous changes, however, it is still not known whether malignant transformation proceeds or results from the near-haploid state. Retrospectively, we have examined 100 metaphases with chromosome counts of 23 to 35 in patients with CML who have not yet progressed to the blastic phase, to see whether such metaphases share any common characteristics with published cases. The unusual behavior of chromosomes 8, 17 and the presence of Ph-chromosomes in 85% of the cells are highly unique features in our study. These observations are compatible with those found in BC/CML patients reported earlier. Therefore, it is hypothesized that selective chromosome loss is a gradual phenomenon and one of these near-haploid clones may replace a diploid clone as the dominant component of the population during blast transformation. Several hypotheses are proposed as to the origin of such clones in malignant hematopoietic stem cells.

摘要

超二倍体在肿瘤性疾病中很常见,但严重的亚二倍体或近单倍体极为罕见。急性淋巴细胞白血病(ALL)和慢性粒细胞白血病的急变期(BC/CML)是最常见的两种白血病,已有报道称在这两种白血病中存在染色体数低至23条的中期细胞。最近的研究表明,在恶性发展过程中,细胞会发生许多变化,然而,恶性转化是由近单倍体状态发展而来还是由其导致,目前仍不清楚。我们回顾性地检查了100个中期细胞,这些细胞来自尚未进展到急变期的慢性粒细胞白血病患者,其染色体数在23至35条之间,以观察这些中期细胞是否与已发表病例有任何共同特征。在我们的研究中,8号、17号染色体的异常行为以及85%的细胞中存在费城染色体是非常独特的特征。这些观察结果与早期报道的BC/CML患者的观察结果一致。因此,有人提出假说,认为选择性染色体丢失是一个渐进的现象,在急变转化过程中,这些近单倍体克隆中的一个可能会取代二倍体克隆,成为群体中的主要成分。关于这些克隆在恶性造血干细胞中的起源,提出了几种假说。

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