AAV-mediated expression of 3TSR inhibits tumor and metastatic lesion development and extends survival in a murine model of epithelial ovarian carcinoma

Darrick L. Yu; Ashley A. Stegelmeier; Natalie Chow; Amira D Rghei; Kathy Matuszewska; Jack Lawler; Byram W. Bridle; Jim Petrik; Sarah K. Wootton

doi:https://doi.org/10.1038/s41417-019-0108-8

doi.org/10.1038/s41417-019-0108-8

AAV-mediated expression of 3TSR inhibits tumor and metastatic lesion development and extends survival in a murine model of epithelial ovarian carcinoma

Darrick L. Yu

5

,

Ashley A. Stegelmeier

6

,

..., Sarah K. Wootton

24

Cancer Gene Therapy6.40

Volume: 27, Issue: 5, Pages: 356 - 367

Published: Jun 4, 2019

Abstract

An integral step in the development of solid tumors is the recruitment of blood vessels to fuel tumor growth. Antiangiogenic therapies can inhibit this process and control solid tumor growth. Thrombospondin-1 is an antiangiogenic protein possessing three type I repeats (3TSR) near the center of the protein and a CD47-binding peptide (CD47) in its C-terminus. Previously, we showed that treatment with recombinant 3TSR induces tumor regression,...

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Paper Details

Title

AAV-mediated expression of 3TSR inhibits tumor and metastatic lesion development and extends survival in a murine model of epithelial ovarian carcinoma

DOI

doi.org/10.1038/s41417-019-0108-8

Published Date

Jun 4, 2019

Journal

Cancer Gene Therapy

Volume

27

Issue

5

Pages

356 - 367

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