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一种新型的含SH2结构域的肌醇磷酸酶剪接形式在髓系发育过程中表达。

A novel spliced form of SH2-containing inositol phosphatase is expressed during myeloid development.

作者信息

Lucas D M, Rohrschneider L R

机构信息

Fred Hutchinson Cancer Research Center, Seattle, WA, USA.

出版信息

Blood. 1999 Mar 15;93(6):1922-33.

Abstract

SH2-containing Inositol Phosphatase (SHIP) is a 145 kD protein expressed in hematopoietic cells. SHIP is phosphorylated on tyrosine after receptor binding by several cytokines and has a negative role in hematopoiesis. We cloned a murine complementary DNA (cDNA) sequence for an isoform of SHIP with an internal 183 nucleotide deletion, encoding a protein 61 amino acids shorter than 145 kD SHIP. This deletion eliminates potential SH3-domain binding regions and a potential binding site for the p85 subunit of Phosphatidylinositol 3-Kinase. Using polyclonal anti-SHIP antibodies, we and others have previously observed a 135 kD SHIP isoform that is coexpressed with 145 kD SHIP. Here, we used monoclonal antibodies raised against the region deleted in the spliced form to show that the product of the novel spliced SHIP cDNA is antigenically identical to the 135 kD SHIP isoform. Like 145 kD SHIP, 135 kD SHIP expression was induced on differentiation of bone marrow cells. After macrophage colony-stimulating factor (M-CSF) stimulation of FDC-P1(Fms) myeloid cells, both 145 and 135 kD SHIP forms were tyrosine phosphorylated and could be coimmunoprecipitated with antibodies to Shc and Grb2. However, experiments showed only a weak association of 135 kD SHIP with p85. A potentially analogous 135 kD SHIP species also appears in human differentiated leukocytes.

摘要

含SH2结构域的肌醇磷酸酶(SHIP)是一种在造血细胞中表达的145 kD蛋白。SHIP在几种细胞因子与受体结合后会发生酪氨酸磷酸化,在造血过程中起负性作用。我们克隆了SHIP一种同工型的小鼠互补DNA(cDNA)序列,该序列内部有183个核苷酸缺失,编码的蛋白质比145 kD的SHIP短61个氨基酸。这种缺失消除了潜在的SH3结构域结合区域以及磷脂酰肌醇3激酶p85亚基的潜在结合位点。我们和其他人之前使用多克隆抗SHIP抗体观察到一种135 kD的SHIP同工型与145 kD的SHIP共表达。在这里,我们使用针对剪接形式中缺失区域产生的单克隆抗体,以表明新剪接的SHIP cDNA产物在抗原性上与135 kD的SHIP同工型相同。与145 kD的SHIP一样,135 kD的SHIP表达在骨髓细胞分化时被诱导。在用巨噬细胞集落刺激因子(M-CSF)刺激FDC-P1(Fms)髓样细胞后,145 kD和135 kD的SHIP形式均发生酪氨酸磷酸化,并且可以与抗Shc和Grb2抗体进行共免疫沉淀。然而,实验表明135 kD的SHIP与p85的结合较弱。一种潜在类似的135 kD的SHIP在人类分化白细胞中也有出现。

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