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Functional dissection of breast cancer risk-associated promoter variants.

Oncotarget. 2017; 
HelbigSonja,WocknerLeesa,BouendeuAnnick,Hille-BetzUrsula,McCueKaren,FrenchJuliet D,EdwardsStacey L,PickettHilda A,ReddelRoger R,Chenevix-TrenchGeorgia,DörkThilo,BeesleyJona
Products/Services Used Details Operation
PCR Cloning and Subcloning Wildtype and variant haplotype TERT promoter sequences (3915bp) harboring all major or all risk-associated alleles of rs2736107, rs2736108, rs145544133, rs2736109, rs3215401 and rs2853669 were synthesized by GenScript and were cloned into a pGL3 reporter vector (Promega E1751). Combinations and single variants were subsequently introduced by cloning fragments containing the variant(s) of interest into the wildtype construct. The constructs were sequence verified after they were obtained from GenScript and following each completed cloning step. Get A Quote

摘要

The multi-cancer susceptibility locus at 5p15.33 includes , encoding the telomerase catalytic subunit. Genome-wide association studies (GWAS) have identified six single nucleotide polymorphisms (SNPs) in the promoter associated with decreased breast cancer risk, although the precise causal variants and their mechanisms of action have remained elusive. Luciferase reporter assays indicated that the protective haplotype reduced promoter activity in human mammary epithelial and cancer cells in an estrogen-independent manner. Using single variant constructs, we identified rs3215401 and rs2853669 as likely functional variants. Silencing of MYC decreased promoter activity but neither MYC nor ETS2 silencing co... More

关键词

GABPA,GWAS,SNP,breast carcinoma,telome