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Frequent induction of chromosomal aberrations in in vivo skin fibroblasts after allogeneic stem cell transplantation: hints to chromosomal instability after irradiation

机译:同种异体干细胞移植后体内皮肤成纤维细胞中染色体畸变的频繁诱导:提示辐射后染色体不稳定

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Total body irradiation (TBI) has been part of standard conditioning regimens before allogeneic stem cell transplantation for many years. Its effect on normal tissue in these patients has not been studied extensively. We studied the in vivo cytogenetic effects of TBI and high-dose chemotherapy on skin fibroblasts from 35 allogeneic stem cell transplantation (SCT) patients. Biopsies were obtained prospectively (n?=?18 patients) before, 3 and 12?months after allogeneic SCT and retrospectively (n?=?17 patients) 23–65 months after SCT for G-banded chromosome analysis. Chromosomal aberrations were detected in 2/18 patients (11?%) before allogeneic SCT, in 12/13 patients (92?%) after 3?months, in all patients after 12?months and in all patients in the retrospective group after allogeneic SCT. The percentage of aberrant cells was significantly higher at all times after allogeneic SCT compared to baseline analysis. Reciprocal translocations were the most common aberrations, but all other types of stable, structural chromosomal aberrations were also observed. Clonal aberrations were observed, but only in three cases they were detected in independently cultured flasks. A tendency to non-random clustering throughout the genome was observed. The percentage of aberrant cells was not different between patients with and without secondary malignancies in this study group. High-dose chemotherapy and TBI leads to severe chromosomal damage in skin fibroblasts of patients after SCT. Our long-term data suggest that this damage increases with time, possibly due to in vivo radiation-induced chromosomal instability.
机译:异体干细胞移植之前,全身照射(TBI)已成为标准条件疗法的一部分。尚未广泛研究其对这些患者的正常组织的作用。我们研究了TBI和大剂量化疗对35名同种异体干细胞移植(SCT)患者皮肤成纤维细胞的体内细胞遗传学作用。在同种异体SCT之前,3和12个月前(n≥17例)进行前瞻性活检(n≥18例),在GCT染色体分析后,在SCT后23-65个月进行回顾性活检(n≥17例)。异基因SCT前2/18的患者(11%),3个月后的12/13患者(92%),12个月后的所有患者以及同种异体后回顾性组的所有患者中检测到染色体畸变SCT。与基线分析相比,异基因SCT后所有时间异常细胞的百分比均显着更高。相互易位是最常见的像差,但也观察到所有其他类型的稳定的结构性染色体像差。观察到了克隆畸变,但只有三例在独立培养的烧瓶中检测到。观察到整个基因组中非随机聚集的趋势。在该研究组中,有和没有继发性恶性肿瘤的患者中异常细胞的百分比没有差异。大剂量化疗和TBI会导致SCT后患者皮肤成纤维细胞中严重的染色体损伤。我们的长期数据表明,这种损害可能会随着时间的推移而增加,这可能是由于体内辐射引起的染色体不稳定所致。

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