Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis

Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis

Abstract Background Angiogenesis is a critical step in the growth of pancreatic neuroendocrine tumors (PNETs) and may be a selective target for PNET therapy. However, PNETs are robustly resistant to current anti-angiogenic therapies that primarily target the VEGFR pathway. Thus, the mechanism of PNE...

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Main Authors: Xi Luo, Jiang-yi He, Jie Xu, Shao-yi Hu, Bang-hui Mo, Qiu-xia Shu, Can Chen, Yu-zhu Gong, Xiao-long Zhao, Gan-feng Xie, Song-tao Yu
Format: Article
Language:English
Published: BMC 2020-09-01
Series:Cell & Bioscience
Subjects:
Neuropilin 2
Angiogenesis
SSH1
Cofilin
Pancreatic neuroendocrine tumor
Online Access:http://link.springer.com/article/10.1186/s13578-020-00472-6
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spelling doaj-df56842489704a90b03463f18da5d5dd2020-11-25T03:21:31ZengBMCCell & Bioscience2045-37012020-09-0110111610.1186/s13578-020-00472-6Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axisXi Luo0Jiang-yi He1Jie Xu2Shao-yi Hu3Bang-hui Mo4Qiu-xia Shu5Can Chen6Yu-zhu Gong7Xiao-long Zhao8Gan-feng Xie9Song-tao Yu10Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Urology, The Second Affiliated Hospital, Third Military Medical University (Army Medical University)Nursing Division, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Thoracic Surgery, Institute of Surgery Research, Daping Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Department of Oncology, Southwest Hospital, Third Military Medical University (Army Medical University)Abstract Background Angiogenesis is a critical step in the growth of pancreatic neuroendocrine tumors (PNETs) and may be a selective target for PNET therapy. However, PNETs are robustly resistant to current anti-angiogenic therapies that primarily target the VEGFR pathway. Thus, the mechanism of PNET angiogenesis urgently needs to be clarified. Methods Dataset analysis was used to identify angiogenesis-related genes in PNETs. Immunohistochemistry was performed to determine the relationship among Neuropilin 2 (NRP2), VEGFR2 and CD31. Cell proliferation, wound-healing and tube formation assays were performed to clarify the function of NRP2 in angiogenesis. The mechanism involved in NRP2-induced angiogenesis was detected by constructing plasmids with mutant variants and performing Western blot, and immunofluorescence assays. A mouse model was used to evaluate the effect of the NRP2 antibody in vivo, and clinical data were collected from patient records to verify the association between NRP2 and patient prognosis. Results NRP2, a VEGFR2 co-receptor, was positively correlated with vascularity but not with VEGFR2 in PNET tissues. NRP2 promoted the migration of human umbilical vein endothelial cells (HUVECs) cultured in the presence of conditioned medium PNET cells via a VEGF/VEGFR2-independent pathway. Moreover, NRP2 induced F-actin polymerization by activating the actin-binding protein cofilin. Cofilin phosphatase slingshot-1 (SSH1) was highly expressed in NRP2-activating cofilin, and silencing SSH1 ameliorated NRP2-activated HUVEC migration and F-actin polymerization. Furthermore, blocking NRP2 in vivo suppressed PNET angiogenesis and tumor growth. Finally, elevated NRP2 expression was associated with poor prognosis in PNET patients. Conclusion Vascular NRP2 promotes PNET angiogenesis by activating the SSH1/cofilin/actin axis. Our findings demonstrate that NRP2 is an important regulator of angiogenesis and a potential therapeutic target of anti-angiogenesis therapy for PNET.http://link.springer.com/article/10.1186/s13578-020-00472-6Neuropilin 2AngiogenesisSSH1CofilinPancreatic neuroendocrine tumor
collection DOAJ
language English
format Article
sources DOAJ
author Xi Luo
Jiang-yi He
Jie Xu
Shao-yi Hu
Bang-hui Mo
Qiu-xia Shu
Can Chen
Yu-zhu Gong
Xiao-long Zhao
Gan-feng Xie
Song-tao Yu
spellingShingle Xi Luo
Jiang-yi He
Jie Xu
Shao-yi Hu
Bang-hui Mo
Qiu-xia Shu
Can Chen
Yu-zhu Gong
Xiao-long Zhao
Gan-feng Xie
Song-tao Yu
Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
Cell & Bioscience
Neuropilin 2
Angiogenesis
SSH1
Cofilin
Pancreatic neuroendocrine tumor
author_facet Xi Luo
Jiang-yi He
Jie Xu
Shao-yi Hu
Bang-hui Mo
Qiu-xia Shu
Can Chen
Yu-zhu Gong
Xiao-long Zhao
Gan-feng Xie
Song-tao Yu
author_sort Xi Luo
title Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
title_short Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
title_full Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
title_fullStr Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
title_full_unstemmed Vascular NRP2 triggers PNET angiogenesis by activating the SSH1-cofilin axis
title_sort vascular nrp2 triggers pnet angiogenesis by activating the ssh1-cofilin axis
publisher BMC
series Cell & Bioscience
issn 2045-3701
publishDate 2020-09-01
description Abstract Background Angiogenesis is a critical step in the growth of pancreatic neuroendocrine tumors (PNETs) and may be a selective target for PNET therapy. However, PNETs are robustly resistant to current anti-angiogenic therapies that primarily target the VEGFR pathway. Thus, the mechanism of PNET angiogenesis urgently needs to be clarified. Methods Dataset analysis was used to identify angiogenesis-related genes in PNETs. Immunohistochemistry was performed to determine the relationship among Neuropilin 2 (NRP2), VEGFR2 and CD31. Cell proliferation, wound-healing and tube formation assays were performed to clarify the function of NRP2 in angiogenesis. The mechanism involved in NRP2-induced angiogenesis was detected by constructing plasmids with mutant variants and performing Western blot, and immunofluorescence assays. A mouse model was used to evaluate the effect of the NRP2 antibody in vivo, and clinical data were collected from patient records to verify the association between NRP2 and patient prognosis. Results NRP2, a VEGFR2 co-receptor, was positively correlated with vascularity but not with VEGFR2 in PNET tissues. NRP2 promoted the migration of human umbilical vein endothelial cells (HUVECs) cultured in the presence of conditioned medium PNET cells via a VEGF/VEGFR2-independent pathway. Moreover, NRP2 induced F-actin polymerization by activating the actin-binding protein cofilin. Cofilin phosphatase slingshot-1 (SSH1) was highly expressed in NRP2-activating cofilin, and silencing SSH1 ameliorated NRP2-activated HUVEC migration and F-actin polymerization. Furthermore, blocking NRP2 in vivo suppressed PNET angiogenesis and tumor growth. Finally, elevated NRP2 expression was associated with poor prognosis in PNET patients. Conclusion Vascular NRP2 promotes PNET angiogenesis by activating the SSH1/cofilin/actin axis. Our findings demonstrate that NRP2 is an important regulator of angiogenesis and a potential therapeutic target of anti-angiogenesis therapy for PNET.
topic Neuropilin 2
Angiogenesis
SSH1
Cofilin
Pancreatic neuroendocrine tumor
url http://link.springer.com/article/10.1186/s13578-020-00472-6
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