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化疗后原发性睾丸非精原细胞瘤与残留成熟畸胎瘤的染色体模式比较。

Comparison of the chromosomal pattern of primary testicular nonseminomas and residual mature teratomas after chemotherapy.

作者信息

van Echten J, van der Vloedt W S, van de Pol M, Dam A, te Meerman G J, Schraffordt Koops H, Sleijfer D T, Oosterhuis J W, de Jong B

机构信息

Department of Medical Genetics, University of Groningen, The Netherlands.

出版信息

Cancer Genet Cytogenet. 1997 Nov;99(1):59-67. doi: 10.1016/s0165-4608(96)00440-2.

Abstract

About 70 to 75% of patients with nonseminomatous testicular germ cell tumors (NSs) present with metastases. When these metastases are treated with chemotherapy, often residual mature teratoma (RMT) is left. RMT is composed of fully differentiated somatic tissue. Untreated metastases of NSs rarely consist exclusively of mature somatic tissue. Apparently, after chemotherapy treatment there is a shift towards higher degrees of differentiation. Investigating tumor progression and the mechanism(s) involved in therapy-related differentiation, we compared the cytogenetically abnormal karyotypes of a series of 70 NSs with those of 31 RMTs. In NSs and RMTs, the modal total chromosome number does not differ and is in the triploid range. Both the frequency and the average copy number of i(12p) are the same, and the pattern of chromosomal over- and underrepresentation and distribution of breakpoints do not differ significantly in these series. So, we found the chromosomal pattern of RMTs as abnormal as those of primary NSs. Based on cytogenetics, we found no indication that specific chromosomal alterations parallel metastasis and therapy-related differentiation of the metastases. The cytogenetic data suggest that both induction of differentiation of (selected) cells or selection of cells with capacity to differentiate are possible mechanisms for the therapy-related differentiation of RMTs.

摘要

约70%至75%的非精原性睾丸生殖细胞肿瘤(NSs)患者存在转移。当这些转移灶接受化疗时,常常会残留成熟畸胎瘤(RMT)。RMT由完全分化的体细胞组织构成。NSs未经治疗的转移灶很少仅由成熟体细胞组织组成。显然,化疗后会出现向更高分化程度的转变。为了研究肿瘤进展以及与治疗相关的分化所涉及的机制,我们比较了一系列70例NSs与31例RMTs的细胞遗传学异常核型。在NSs和RMTs中,核型的总染色体数模式并无差异,且处于三倍体范围内。i(12p)的频率和平均拷贝数相同,这些系列中染色体增减现象的频率以及断点的分布也无显著差异。因此,我们发现RMTs的染色体模式与原发性NSs的一样异常。基于细胞遗传学,我们未发现特定染色体改变与转移以及转移灶的治疗相关分化平行的迹象。细胞遗传学数据表明,(选定)细胞分化的诱导或具有分化能力细胞的选择可能是RMTs治疗相关分化的机制。

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