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Tumor microvasculature and microenvironment: Targets for anti-angiogenesis and normalization

期刊

MICROVASCULAR RESEARCH
卷 74, 期 2-3, 页码 72-84

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.mvr.2007.05.003

关键词

angiogenesis; lymphangiogenesis; tumor; stromal cells; vascular endothelial growth factor; microenvironment; hypoxia; acidosis; interstitial fluid pressure; metastasis

资金

  1. NATIONAL CANCER INSTITUTE [R35CA056591, R24CA085140, P01CA080124, U01CA084301, R01CA096915, R01CA085140, R01CA115767] Funding Source: NIH RePORTER
  2. NCI NIH HHS [U01 CA084301, R01 CA096915-01, P01 CA080124-04, R24 CA085140-03, P01 CA080124-07, R01 CA096915-03, U01 CA084301-09, P01 CA080124-020001, P01-CA-80124, R24 CA085140, U01-CA084301, P01 CA080124-049003, P01 CA080124-02, R01 CA096915-05, R01 CA085140-07, P01 CA080124-050001, R24 CA085140-01, P01 CA080124-039003, P01 CA080124-040001, U01 CA084301-07, R01 CA096915-02, P01 CA080124-06A25967, P01 CA080124-01A19003, P01 CA080124-05S10001, R01 CA085140, R24 CA085140-05, P01 CA080124-01A1S19003, R01 CA085140-08, R01 CA096915, P01 CA080124-05, R01 CA115767-02, R24 CA085140-02, R24 CA085140-04, R01-CA11576-01, P01 CA080124, P01 CA080124-029003, P01 CA080124-03, P01 CA080124-01A10001, R01 CA115767-01A1, P01 CA080124-06A25972, U01 CA084301-08, P01 CA080124-059003, U01 CA084301-06, P01 CA080124-06A2, P01 CA080124-01A1, R01-CA85140, P01 CA080124-01A1S10001, P01 CA080124-030001, R01-CA96915, R01 CA085140-06, R35 CA056591-07, P01 CA080124-05S19003, R01 CA115767, R01 CA096915-04] Funding Source: Medline

向作者/读者索取更多资源

A solid tumor forms an organ-like entity comprised of neoplastic cells and non-transformed host stromal cells embedded in an extracellular matrix. Similar to normal tissues, blood vessels nourish cells residing in tumors. However, unlike normal blood vessels, tumor vasculature has abnormal organization, structure, and function. Tumor vessels are leaky and blood flow is heterogeneous and often compromised. Vascular hyperpermeability and the lack of functional lymphatic vessels inside tumors cause elevation of interstitial fluid pressure in solid tumors. Each of these abnormalities forms a physiological barrier to the delivery of therapeutic agents to tumors. Furthermore, elevated tumor interstitial fluid pressure increases fluid flow from the tumor margin into the peri-tumor area and may facilitate peri-tumor lymphatic hyperplasia and metastasis. Abnormal microcirculation in tumors also leads to a hostile microenvironment characterized by hypoxia and acidosis, which hinder the effectiveness of anti-tumor treatments such as radiation therapy and chemotherapy. In addition, host-tumor interactions regulate expression of pro- and anti-angiogenic factors and hence contribute to their imbalance and resulting pathophysiological characteristics of the tumor. Restoration of pro- and anti-angiogenic balance in tumors may normalize tumor vasculature and thus improve its function. Indeed, anti-angiogenic treatments directly targeting angiogenic signaling pathways as well as indirectly modulating angiogenesis show normalization of tumor vasculature and microenvironment at least transiently in both preclinical and clinical settings. Combination of cytotoxic therapy and anti-angiogenic treatment during the vascular normalization exhibits synergistic effect. (C) 2007 Elsevier Inc. All rights reserved.

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