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在小细胞肺癌中鉴定出的神经元型钙通道的分子多样性。

Molecular diversity of neuronal-type calcium channels identified in small cell lung carcinoma.

作者信息

Oguro-Okano M, Griesmann G E, Wieben E D, Slaymaker S J, Snutch T P, Lennon V A

机构信息

Department of Immunology, Mayo Clinic, Rochester, MN 55905.

出版信息

Mayo Clin Proc. 1992 Dec;67(12):1150-9. doi: 10.1016/s0025-6196(12)61144-6.

Abstract

Using the polymerase chain reaction (PCR), we identified RNA transcripts for two distinct classes of neuronal-type voltage-gated Ca2+ channels (VGCC) in a prototypic small cell lung carcinoma (SCLC) cell line, SCC-9. Oligonucleotide primers were designed to encode amino acid sequences common to alpha 1-subunits of known neuronal VGCC classes. Sequencing of complementary DNA (cDNA) clones derived from two independent PCR products revealed that one corresponded to a brain class A VGCC fragment predicted to encode a P-type VGCC (insensitive to dihydropyridines and omega-conotoxin) characteristic of cerebellar Purkinje cells but not previously identified in humans. The second PCR product was identical (except for one conservative nucleotide difference) to a fragment of the class D VGCC of neurons and neuroendocrine cells, which encodes an L-type VGCC (sensitive to dihydropyridines). By Northern blot analyses, both cDNAs hybridized to messenger RNAs (mRNAs) obtained from SCC-9; class D hybridized additionally to human cerebral cortical mRNA, but neither hybridized to mRNA from the skeletal muscle cell line TE671. Although no cDNA corresponding to class B VGCC (N-type) was identified, SCLCs are known to express VGCC that are sensitive to omega-conotoxin and coprecipitate with 125I-labeled-omega-conotoxin when complexed with serum IgG from patients with the Lambert-Eaton myasthenic syndrome. The multiple classes of neuronal-type VGCC expressed in SCLC could conceivably have both unique and related antigenic determinants that may give rise to antineuronal autoimmune responses. This would account for a spectrum of paraneoplastic neurologic disorders including the Lambert-Eaton syndrome and subacute cerebellar degeneration.

摘要

利用聚合酶链反应(PCR),我们在一种典型的小细胞肺癌(SCLC)细胞系SCC - 9中鉴定出了两类不同的神经元型电压门控钙通道(VGCC)的RNA转录本。设计了寡核苷酸引物来编码已知神经元VGCC类别的α1亚基共有的氨基酸序列。对来自两个独立PCR产物的互补DNA(cDNA)克隆进行测序,结果显示其中一个对应于脑A类VGCC片段,预计编码一种P型VGCC(对二氢吡啶和ω - 芋螺毒素不敏感),这是小脑浦肯野细胞的特征,但此前在人类中未被鉴定出来。第二个PCR产物与神经元和神经内分泌细胞的D类VGCC片段相同(除了一个保守的核苷酸差异),该片段编码一种L型VGCC(对二氢吡啶敏感)。通过Northern印迹分析,两种cDNA都与从SCC - 9获得的信使RNA(mRNA)杂交;D类还与人类大脑皮质mRNA杂交,但两者都不与骨骼肌细胞系TE671的mRNA杂交。尽管未鉴定出与B类VGCC(N型)对应的cDNA,但已知SCLC表达对ω - 芋螺毒素敏感的VGCC,并且当与来自兰伯特 - 伊顿肌无力综合征患者的血清IgG复合时,会与125I标记的ω - 芋螺毒素共沉淀。SCLC中表达的多种神经元型VGCC可能具有独特的和相关的抗原决定簇,这可能引发抗神经元自身免疫反应。这可以解释一系列副肿瘤性神经系统疾病,包括兰伯特 - 伊顿综合征和亚急性小脑变性。

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