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PTBP1-Mediated Alternative Splicing Regulates the Inflammatory Secretome and the Pro-tumorigenic Effects of Senescent Cells.

Cancer Cell. 2018; 
Georgilis Athena,Klotz Sabrina,Hanley Christopher J,Herranz Nicolas,Weirich Benedikt,Morancho Beatriz,Leote Ana Carolina,D'Artista Luana,Gallage Suchira,Seehawer Marco,Carroll Thomas,Dharmalingam Gopuraja,Wee Keng Boon,Mellone Marco,Pombo Joaquim,Heide Danijela,Guccione Ernesto,Arribas Joaquín,Barbosa-Morais Nuno L,Heikenwalder Mathias,Thomas Gareth J,Zender Lars,Gil Je
Products/Services Used Details Operation
Custom Vector Construction 4) was PCR amplified from pBABE-PTBP1 vector custom-synthesised by GenScript, using primers CMVPTBP1F (5’-CGTTCGAAGCCACCATGGACGG CATTGTCCCA-3’) and CMVPTBP1R (5’-CCGGTTTAAACCTAGATGGTGGACTTGGAGAAG-3’), and the PlatinumÒ PCR SuperMix High Fidelity (Invitrogen) according to manufacturer’s instructions. Get A Quote

摘要

Oncogene-induced senescence is a potent tumor-suppressive response. Paradoxically, senescence also induces an inflammatory secretome that promotes carcinogenesis and age-related pathologies. Consequently, the senescence-associated secretory phenotype (SASP) is a potential therapeutic target. Here, we describe an RNAi screen for SASP regulators. We identified 50 druggable targets whose knockdown suppresses the inflammatory secretome and differentially affects other SASP components. Among the screen candidates was PTBP1. PTBP1 regulates the alternative splicing of genes involved in intracellular trafficking, such as EXOC7, to control the SASP. Inhibition of PTBP1 prevents the pro-tumorigenic effects of... More

关键词

EXOC7,Oncogene-induced senescence,PTBP1,RNAi screen,SASP,alternative splicing,senesc