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Identification of mutations in the coding sequence of the proto-oncogene c-kit in a human mast cell leukemia cell line causing ligand-independent activation of c-kit product.

机译：鉴定人肥大细胞白血病细胞系中原癌基因c-kit编码序列中的突变，从而引起c-kit产品的配体非依赖性活化。

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The c-kit proto-oncogene encodes a receptor tyrosine kinase. Binding of c-kit ligand, stem cell factor (SCF) to c-kit receptor (c-kitR) is known to activate c-kitR tyrosine kinase, thereby leading to autophosphorylation of c-kitR on tyrosine and to association of c-kitR with substrates such as phosphatidylinositol 3-kinase (PI3K). In a human mast cell leukemia cell line HMC-1, c-kitR was found to be constitutively phosphorylated on tyrosine, activated, and associated with PI3K without the addition of SCF. The expression of SCF mRNA transcript in HMC-1 cells was not detectable by means of PCR after reverse transcription (RT-PCR) analysis, suggesting that the constitutive activation of c-kitR was ligand independent. Sequencing of whole coding region of c-kit cDNA revealed that c-kit genes of HMC-1 cells were composed of a normal, wild-type allele and a mutant allele with two point mutations resulting in intracellular amino acid substitutions of Gly-560 for Val and Val-816 for Asp. Amino acid sequences in the regions of the two mutations are completely conserved in all of mouse, rat, and human c-kit. In order to determine the causal role of these mutations in the constitutive activation, murine c-kit mutants encoding Gly-559 and/or Val-814, corresponding to human Gly-560 and/or Val-816, were constructed by site-directed mutagenesis and expressed in a human embryonic kidney cell line, 293T cells. In the transfected cells, both c-kitR (Gly-559, Val-814) and c-kitR (Val-814) were abundantly phosphorylated on tyrosine and activated in immune complex kinase reaction in the absence of SCF, whereas tyrosine phosphorylation and activation of c-kitR (Gly-559) or wild-type c-kitR was modest or little, respectively. These results suggest that conversion of Asp-816 to Val in human c-kitR may be an activating mutation and responsible for the constitutive activation of c-kitR in HMC-1 cells.

机译：c-kit原癌基因编码受体酪氨酸激酶。已知c-kit配体，干细胞因子（SCF）与c-kit受体（c-kitR）的结合可激活c-kitR酪氨酸激酶，从而导致c-kitR在酪氨酸上自磷酸化并与c-kitR缔合带有磷脂酰肌醇3-激酶（PI3K）等底物。在人类肥大细胞白血病细胞系HMC-1中，发现在不添加SCF的情况下c-kitR在酪氨酸上组成性磷酸化，活化并与PI3K相关。在逆转录（RT-PCR）分析后，无法通过PCR检测到HMC-1细胞中SCF mRNA转录的表达，这表明c-kitR的组成性激活是独立于配体的。对c-kit cDNA整个编码区的测序表明，HMC-1细胞的c-kit基因由正常的野生型等位基因和具有两个点突变的突变等位基因组成，导致Gly-560的胞内氨基酸取代。 Val和Asp的Val-816。两个突变区域中的氨基酸序列在所有小鼠，大鼠和人类c-kit中都完全保守。为了确定这些突变在组成性激活中的因果作用，通过定点构建了编码Gly-559和/或Val-814的鼠类c-kit突变体（对应于人Gly-560和/或Val-816）诱变并在人类胚胎肾细胞系293T细胞中表达。在转染的细胞中，c-kitR（Gly-559，Val-814）和c-kitR（Val-814）都在酪氨酸上大量磷酸化，并在没有SCF的情况下在免疫复合激酶反应中被激活，而酪氨酸磷酸化和激活c-kitR（Gly-559）或野生型c-kitR分别适度或很少。这些结果表明，人c-kitR中Asp-816向Val的转化可能是激活突变，并负责HMC-1细胞中c-kitR的组成性激活。

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作者
Furitsu, T; Tsujimura, T; Tono, T; Ikeda, H; Kitayama, H; Koshimizu, U; Sugahara, H; Butterfield, J H; Ashman, L K; Kanayama, Y;
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年度 1993
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专利

1. Mast cell leukemia: Identification of a new c-Kit mutation, dup(501-502), and response to masitinib, a c-Kit tyrosine kinase inhibitor [J] . Georgin-LavialleS., LhermitteL., SuarezF., European Journal of Haematology . 2012,第1期

机译：肥大细胞白血病：识别新的c-Kit突变dup（501-502）和对c-Kit酪氨酸激酶抑制剂马赛替尼的反应
2. Clustering of activating mutations in c-KIT's juxtamembrane coding region in canine mast cell neoplasms. [J] . Ma Y, Longley BJ, Wang X, The Journal of investigative dermatology. . 1999,第2期

机译：犬肥大细胞肿瘤中c-KIT近膜编码区中激活突变的聚类。
3. Activating mutations of c-kit at codon 816 confer drug resistance in human leukemia cells. [J] . Ning ZQ, Li J, Arceci RJ Leukemia and lymphoma . 2001,第5a6期

机译：c-kit密码子816的激活突变赋予人白血病细胞耐药性。
4. Regulation of c-Kit Expression In Human Mast Cells Inhibition of SCF-fnduced c-Kit Downregulation by STI 571 (Gleevec) in LAD 2 and HMC-1 Cells [C] . M. Babina, C. Rex, S. Guhl, Collegium Internationale Allergologicum . 2007

机译：在LAD 2和HMC-1细胞中，在人肥大细胞中抑制SCF-Fnduced C-kit的抑制C-kit的调节抑制STI 571（GLEEVEC）和HMC-1细胞
5. The role of c-KIT mutations in tumorigenesis in humans and dogs [D] . Thaiwong, Tuddow 2012

机译：c-KIT突变在人和狗的肿瘤发生中的作用
6. Identification of mutations in the coding sequence of the proto-oncogene c-kit in a human mast cell leukemia cell line causing ligand-independent activation of c-kit product. [O] . T Furitsu, T Tsujimura, T Tono, 1993

机译：鉴定人肥大细胞白血病细胞系中原癌基因c-kit编码序列中的突变从而引起c-kit产品的配体非依赖性活化。
7. Functional and phenotypic studies of two variants of a human mast cell line with a distinct set of mutations in the c-kit proto-oncogene [O] . Sundström, Magnus, Vliagoftis, Harissios, Karlberg, Peter, 2003

机译：对人类肥大细胞系的两个变体进行功能和表型研究，该变体在c-kit原癌基因中具有独特的突变集

Identification of mutations in the coding sequence of the proto-oncogene c-kit in a human mast cell leukemia cell line causing ligand-independent activation of c-kit product.

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