资源 » 参考数据库 » 客户发表文献

至今,GenScript的服务及产品已被Cell, Nature, Science, PNAS等1300多家生物医药类杂志引用近万次,处于行业领先水平。NIH、哈佛、耶鲁、斯坦福、普林斯顿、杜克大学等约400家全球著名机构使用GenScript的基因合成、多肽服务、抗体服务和蛋白服务等成功地发表科研成果,再次证明GenScript 有能力帮助业内科学家Make research easy.

Restoring RUNX1 deficiency in RUNX1 familial platelet disorder by inhibiting its degradation

Blood Adv. 2021-02; 
Michelle C Krutein, Matthew R Hart, Donovan J Anderson, Jasmin Jeffery, Andriana G Kotini, Jin Dai, Sylvia Chien, Michaela DelPriore, Sara Borst, Jean Ann Maguire, Deborah L French, Paul Gadue, Eirini P Papapetrou, Siobán B Keel, Pamela S Becker, Marshall S Horwitz
Products/Services Used Details Operation
Mammalian Expression Human RUNX1 variant-1 cDNA (NM_001754.3) with carboxyl-terminal FLAG epitope tag in pcDNA3.1 vector (pcDNA3.1-RUNX1–FLAG) was purchased from Genscript (OHu26363). Get A Quote

摘要

RUNX1 familial platelet disorder (RUNX1-FPD) is an autosomal dominant disorder caused by a monoallelic mutation of RUNX1, initially resulting in approximately half-normal RUNX1 activity. Clinical features include thrombocytopenia, platelet functional defects, and a predisposition to leukemia. RUNX1 is rapidly degraded through the ubiquitin-proteasome pathway. Moreover, it may autoregulate its expression. A predicted kinetic property of autoregulatory circuits is that transient perturbations of steady-state levels result in continued maintenance of expression at adjusted levels, even after inhibitors of degradation or inducers of transcription are withdrawn, suggesting that transient inhibition of RUNX1 degradat... More

关键词

Article Link >