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Frequent β‐Catenin Abnormalities in Bone and Soft‐tissue Tumors

机译:骨和软组织肿瘤中常见的β-Catenin异常

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摘要

We have screened mutations of the β‐catenin gene by using the polymerase chain reaction‐single strand conformation polymorphism (PCR‐SSCP) method in 62 malignant bone and soft‐tissue tumors, including malignant fibrous histiocytomas (MFHs), osteosarcomas, synovial sarcomas, liposarcomas, malignant schwannomas, and other types of tumors, as well as 11 benign tumors. β‐Catenin‐activating missense mutations were found in two malignant tumors. One found in MFH occurred at codon 45 and caused an amino acid substitution from serine (one of the GSK3β‐targeted phosphorylation sites) to phenylalanine. The other, detected in synovial sarcoma at codon 32, resulted in an amino acid change from aspartic acid (located adjacent to the phosphorylation target, serine, encoded by codon 33) to tyrosine. Furthermore, we found accumulation of β‐catenin by western‐blotting analysis in 12 of 19 malignant tumors in which we found no mutation involving exon 3. Our results suggested the possible involvement of β‐catenin activation, by β‐catenin gene mutation or alteration of other factor(s), in the formation and/or progression of various types of bone and soft‐tissue tumors.
机译:我们使用聚合酶链反应-单链构象多态性(PCR-SSCP)方法筛选了62种恶性骨和软组织肿瘤中β-catenin基因的突变,包括恶性纤维组织细胞瘤(MFHs),骨肉瘤,滑膜肉瘤,脂肪肉瘤,恶性神经鞘瘤和其他类型的肿瘤,以及11种良性肿瘤。在两个恶性肿瘤中发现了β-连环蛋白激活的错义突变。在MFH中发现的一个发生在第45位密码子处,并导致氨基酸从丝氨酸(GSK3β靶向的磷酸化位点之一)变为苯丙氨酸。在滑膜肉瘤中第32位密码子中检测到的另一个氨基酸导致了氨基酸的变化,从天冬氨酸(位于磷酸化靶标丝氨酸旁边,由密码子33编码)变为酪氨酸。此外,我们通过western印迹分析发现了19个恶性肿瘤中的12个,其中未发现涉及外显子3突变的β-catenin积累。我们的结果表明,β-catenin基因突变或改变可能与β-catenin激活有关。各种类型的骨和软组织肿瘤的形成和/或发展过程中的其他因素。

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