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Loss of Wild-Type MEN1 Gene Expression in Multiple Endocrine Neoplasia Type 1-Associated Parathyroid Adenoma

机译:多型内分泌肿瘤1型相关甲状旁腺腺瘤中野生型MEN1基因表达的损失。

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References(13) Cited-By(3) Multiple endocrine neoplasia type 1(MEN1) is a human hereditary tumor syndrome characterized by the development of endocrine adenomas of the parathyroid, anterior pituitary, and enteropancreatic tissue. Several lines of evidence have implicated the recently identified MEN1 gene located on chromosome 11q13 as a recessive tumor suppressor gene. Here, we analyzed MEN1 wild-type gene expression in tumors from a large MEN1 kindred. A deletion of codons 227-228 (678de16) located in exon 4 was found in tumor and peripheral blood complementary DNA using a simplified single-strand conformational polymorphism (SSCP) approach well suited for clinical MEN1 mutation screening. The identified 678de16 cDNA mutation deletes a potential phosphorylation site (Tyr227) and corresponds to a germ line mutation co-segregating with disease phenotype in this MEN1 family. Loss of heterozygosity analysis by fluorescent microsatellite PCR showed an exclusive loss of the MEN1 wild-type (and retention of the mutated) allele detectable in DNA from microdissected parathyroid and pancreatic, but not in adrenal, adenomas. Our findings confirm the synergism between MEN1 gene mutations and subsequent MEN1 allelic losses in the tumorigenesis of MEN1-associated adenomas.
机译:参考文献(13)被引用的By(3)多发性内分泌肿瘤1型(MEN1)是一种人类遗传性肿瘤综合征,其特征是甲状旁腺,垂体前叶和肠胰组织的内分泌腺瘤发展。几条证据表明,最近鉴定出的位于染色体11q13上的MEN1基因是隐性肿瘤抑制基因。在这里,我们分析了MEN1野生型基因在来自大型MEN1家族的肿瘤中的表达。使用简化的单链构象多态性(SSCP)方法在肿瘤和外周血互补DNA中发现了位于外显子4上的密码子227-228(678de16)的缺失,非常适合临床MEN1突变筛查。鉴定出的678de16 cDNA突变删除了一个潜在的磷酸化位点(Tyr227),并与该MEN1家族中与疾病表型共分离的种系突变相对应。通过荧光微卫星PCR进行的杂合性丧失分析显示,在微小解剖的甲状旁腺和胰腺组织的DNA中可检测到MEN1野生型(保留突变的)等位基因,但在肾上腺腺瘤中却没有。我们的发现证实了MEN1相关腺瘤的肿瘤发生中MEN1基因突变与随后的MEN1等位基因缺失之间的协同作用。

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