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人胶质母细胞瘤中20S蛋白酶体的特征分析。

Characterization of the 20S proteasome in human glioblastomas.

作者信息

Piccinini Marco, Rinaudo Maria Teresa, Anselmino Annalisa, Ramondetti Cristina, Buccinnà Barbara, Fiano Valentina, Ghimenti Chiara, Schiffer Davide

机构信息

Department of Medicine and Experimental Oncology, Section of Biochemistry, University of Turin, Via Michelangelo n 27/b, 10126 Turin, Italy.

出版信息

Anticancer Res. 2005 Sep-Oct;25(5):3203-10.

Abstract

Proteasomes are multisubunit proteases involved in many cellular processes, including tumorigenesis and immune surveillance. In their catalytic core, the 20S proteasome, the beta1, beta2 and beta5 subunits show peptidylglutamyl peptide hydrolyzing (PGPH), trypsin-like and chymotrypsin-like activities, respectively. By IFN-gamma and TNFalpha stimulus, these subunits are replaced by their counterparts LMP2, MECL-1 and LMP7, defined inducible subunits, thus originating the immunoproteasome, and expression of the proteasome activator PA28 is enhanced. These modifications strengthen MHC-class I restricted peptide generation. The 20S proteasome has been detected immunohistochemically in formalin-fixed samples purified from fresh surgical specimens of 18 tumors (G20S) and from 8 samples of normal peritumoral tissue. The G20S, LMP2, MECL-1 and LMP7 increased in only 12 cases, along with unvaried trypsin-like and decreased PGPH and chymotrypsin-like activities; PA28 was unvaried in all 18 samples. The immunoproteasome alterations may represent an anomalous immunological attitude of glioblastomas.

摘要

蛋白酶体是参与许多细胞过程的多亚基蛋白酶,包括肿瘤发生和免疫监视。在其催化核心20S蛋白酶体中,β1、β2和β5亚基分别表现出肽基谷氨酰肽水解(PGPH)、胰蛋白酶样和糜蛋白酶样活性。通过γ干扰素和肿瘤坏死因子α刺激,这些亚基被其对应物LMP2、MECL-1和LMP7取代,这些对应物被定义为诱导性亚基,从而产生免疫蛋白酶体,并且蛋白酶体激活剂PA28的表达增强。这些修饰增强了MHC-I类限制性肽的产生。在从18个肿瘤的新鲜手术标本(G20S)和8个正常肿瘤周围组织样本中纯化的福尔马林固定样本中,通过免疫组织化学检测到了20S蛋白酶体。G20S、LMP2、MECL-1和LMP7仅在12例中增加,同时胰蛋白酶样活性不变,PGPH和糜蛋白酶样活性降低;PA28在所有18个样本中均无变化。免疫蛋白酶体改变可能代表胶质母细胞瘤异常的免疫状态。

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