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五例经手术治疗的腰骶部脊索瘤的细胞遗传学、端粒和端粒酶研究

Cytogenetic, telomere, and telomerase studies in five surgically managed lumbosacral chordomas.

作者信息

Butler M G, Dahir G A, Hedges L K, Juliao S F, Sciadini M F, Schwartz H S

机构信息

Division of Genetics, Vanderbilt University School of Medicine, Nashville, Tennesse 37232-2578, USA.

出版信息

Cancer Genet Cytogenet. 1995 Nov;85(1):51-7. doi: 10.1016/0165-4608(95)00127-1.

Abstract

Lumbosacral chordomas are rare skeletal sarcomas of the spine that originate from the remnant notochord. The understanding of this human cancer is limited to observations of its clinical behavior and its embryonic link. Thus, we performed chromosome and molecular analyses from five surgically harvested chordomas in an effort to document genetic and biochemical abnormalities which might aid in understanding the tumor biology of this understudied neoplasm. Cytogenetic analysis of the five chordomas revealed normal results in four patients and random abnormalities in only one tumor cell in the 100 cells studied from the fifth patient. A repeat telomeric probe (TTAGGG)50 was hybridized to genomic DNA isolated from chordoma cells (and HeLa cells) and digested with HinfI. The tumor DNA was paired with leukocyte DNA from age-matched controls and revealed telomere elongation in four of the four chordoma patients studied with molecular genetic techniques. Conversely, telomere length reduction has been reported during in vitro senescence of human fibroblasts, giant cell tumor of bone, colon cancer, intracranial tumors, childhood leukemia, Wilms tumor, and in HeLa cells. Telomerase activity (telomerase is required to maintain telomere integrity) was also determined by visualizing the extension of radioactive telomeric repeats on DNA sequencing gels. The telomeric fragments were assembled during incubation of the cytoplasmic extract containing telomerase. Telomerase activity was observed in HeLa (positive control and commercially available cell line), giant cell tumor of bone (positive control tumor cells from living patients), and in chordoma cells from one of the two chordoma patients (but to a lesser degree compared with HeLa). As expected, the chordoma patients' fibroblasts exhibited no telomerase activity.

摘要

腰骶部脊索瘤是一种罕见的脊柱骨骼肉瘤,起源于残留的脊索。对这种人类癌症的了解仅限于对其临床行为及其胚胎学联系的观察。因此,我们对五例手术切除的脊索瘤进行了染色体和分子分析,以记录可能有助于理解这种研究较少的肿瘤生物学的遗传和生化异常情况。对这五例脊索瘤的细胞遗传学分析显示,四例患者结果正常,在对第五例患者研究的100个细胞中,仅一个肿瘤细胞出现随机异常。将重复端粒探针(TTAGGG)50与从脊索瘤细胞(和HeLa细胞)中分离的基因组DNA杂交,并用HinfI消化。将肿瘤DNA与年龄匹配对照的白细胞DNA配对,通过分子遗传学技术研究发现,四例脊索瘤患者中有四例出现端粒延长。相反,据报道,在人类成纤维细胞、骨巨细胞瘤、结肠癌、颅内肿瘤、儿童白血病、肾母细胞瘤的体外衰老过程中以及在HeLa细胞中,端粒长度会缩短。还通过在DNA测序凝胶上观察放射性端粒重复序列的延伸来测定端粒酶活性(维持端粒完整性需要端粒酶)。在含有端粒酶的细胞质提取物孵育过程中组装端粒片段。在HeLa细胞(阳性对照和市售细胞系)、骨巨细胞瘤(来自活体患者的阳性对照肿瘤细胞)以及两名脊索瘤患者之一的脊索瘤细胞中观察到端粒酶活性(但与HeLa细胞相比程度较低)。正如预期的那样,脊索瘤患者的成纤维细胞未表现出端粒酶活性。

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