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Human hyaluromdases map to a candidate tumor suppressor Iocus

机译:人透明质酸酶定位到候选肿瘤抑制物

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Eukaryotic hyaluronidases are widely distributed, but until recently the only vertebrate enzyme to be cloned was the sperm-specific enzyme, PH20. We have now purified the hyaluronidase of human plasma. The identical enzyme, as well as a second proteolytically processed form, is present in urine. Amino acid sequence of the purified hyaluronidase matched a cDNA in the human Expressed Sequence Tag database which, in combination with 5'-RACE-PCR, was used to clone the gene. termed HYALI, coding for a protein of 435 amino acids. HYALI is identical to an uncharacterized gene positionally cloned by others at chromosome 3p21.3 that is homozygously deleted in several small cell lung careinoma cell lines. We have also identified two additional paralogous hyaluronidase-like genes flanking HYAL1 on chromosome 3p21.3 termed HYAL2 and HYAL3. We are evaluating the candidacy of these two genes as potential tumor suppressors. The mouse hyaluronidase gene, by convention termed Hyall, was also cloned and expressed and found to be 73 identical to the human enzyme. In mouse, serum hyaluronidase polymorphism has previously been mapped to 60 cM from the centromere of chromosome 9, which corresponds to a cytogenetic location of gFI-F2, a region syntenic to the human 3pZ1.3. Mice with alleles of Hyall producing higher levels of plasma hyaluronidase have greater resistance to transplanted tumor growth. products of these candidate tumor suppressor genes are being evaluated as potential anticancer agents.
机译:真核透明质酸酶广泛分布,但是直到最近,唯一要克隆的脊椎动物酶是精子特异性酶PH20。现在,我们已经纯化了人血浆的透明质酸酶。尿液中存在相同的酶以及第二种蛋白水解加工形式。纯化的透明质酸酶的氨基酸序列与人表达序列标签数据库中的cDNA相匹配,该数据库与5'-RACE-PCR一起用于克隆基因。称为HYALI,可编码435个氨基酸的蛋白质。 HYALI与由其他人克隆在3p21.3号染色体上的一个未表征的基因相同,该基因在几种小细胞肺转移瘤细胞系中被纯合缺失。我们还确定了在染色体3p21.3上位于HYAL1侧翼的两个另外的同源透明质酸酶样基因,称为HYAL2和HYAL3。我们正在评估这两个基因作为潜在的抑癌基因的候选资格。小鼠透明质酸酶基因,按照惯例被称为Hyall,也被克隆并表达,发现与人类酶具有73个相同性。在小鼠中,血清透明质酸酶的多态性先前已被定位到9号染色体着丝粒的60 cM处,这对应于gFI-F2的细胞遗传学位置,该区域与人3pZ1.3同源。具有Hyall等位基因的小鼠产生更高水平的血浆透明质酸酶,对移植瘤的生长具有更大的抵抗力。这些候选肿瘤抑制基因的产物被评估为潜在的抗癌药。

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