| Literature DB >> 26243191 |
Kelly Foley1, Agnieszka A Rucki1, Qian Xiao2, Donger Zhou2, Ashley Leubner2, Guanglan Mo3, Jennifer Kleponis2, Annie A Wu2, Rajni Sharma4, Qingguang Jiang5, Robert A Anders6, Christine A Iacobuzio-Donahue6, Katherine A Hajjar7, Anirban Maitra6, Elizabeth M Jaffee8, Lei Zheng9.
Abstract
Most patients with pancreatic ductal adenocarcinoma (PDA) present with metastatic disease at the time of diagnosis or will recur with metastases after surgical treatment. Semaphorin-plexin signaling mediates the migration of neuronal axons during development and of blood vessels during angiogenesis. The expression of the gene encoding semaphorin 3D (Sema3D) is increased in PDA tumors, and the presence of antibodies against the pleiotropic protein annexin A2 (AnxA2) in the sera of some patients after surgical resection of PDA is associated with longer recurrence-free survival. By knocking out AnxA2 in a transgenic mouse model of PDA (KPC) that recapitulates the progression of human PDA from premalignancy to metastatic disease, we found that AnxA2 promoted metastases in vivo. The expression of AnxA2 promoted the secretion of Sema3D from PDA cells, which coimmunoprecipitated with the co-receptor plexin D1 (PlxnD1) on PDA cells. Mouse PDA cells in which SEMA3D was knocked down or ANXA2-null PDA cells exhibited decreased invasive and metastatic potential in culture and in mice. However, restoring Sema3D in AnxA2-null cells did not entirely rescue metastatic behavior in culture and in vivo, suggesting that AnxA2 mediates additional prometastatic mechanisms. Patients with primary PDA tumors that have abundant Sema3D have widely metastatic disease and decreased survival compared to patients with tumors that have relatively low Sema3D abundance. Thus, AnxA2 and Sema3D may be new therapeutic targets and prognostic markers of metastatic PDA.Entities:
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Year: 2015 PMID: 26243191 PMCID: PMC4811025 DOI: 10.1126/scisignal.aaa5823
Source DB: PubMed Journal: Sci Signal ISSN: 1945-0877 Impact factor: 8.192