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The prothrombotic state in cancer

  • ,
  • Lluvia Sugey Sosa-Quinteroe(Author)
    ,
  • Sandra Guzmán-Silahuae(Author)
    ,
  • Eduardo García-Lunab(Author)
    ,
  • Carlos Riebeling-Navarroc, d(Author)
    ,
  • Arnulfo Hernán Nava-Zavalae, f, g(Author)
  • ,
  • bUniversidad de Monterrey
    ,
  • cInstituto Mexicano del Seguro Social
    ,
  • dUniversidad Nacional Autónoma de México
    ,
  • eHospital de Especialidades
    ,
  • fHospital General de Occidente
Research Output: Chapter in Book/Report/Conference proceeding Chapter

Sustainable Development Goals

  • SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well

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36
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Abstract

Neoplasms result from changes in the mechanisms of growth, differentiation, and cellular death. Cancers are of high clinical relevance due to their prevalence and associated morbidity and mortality. The clinical and biological diversity of cancer depends mainly on cellular origin and degree of differentiation. These changes result from alterations in molecular expression that generate a complex clinical, biochemical, and morphologic phenotype. Although cancer is associated with a hypercoagulable state, few cancers result in a thrombotic event. Many factors influence thrombotic incidence, such as advanced disease, central catheter placement, chemotherapy, neoplasia, and surgery. The pro-coagulant state is associated with anomalies in the vascular wall, blood flow, blood constituents (tissue factor, thrombin), coagulation state, and cell growth factors. Tumor cells perpetuate this phenomenon by releasing tissue factor, inflammatory cytokines, and growth factors. These changes favor cellular activation that gives rise to actions involving coagulation, inflammation, thrombosis, tumor growth, angiogenesis, and tumor metastases. These, in turn, are closely linked to treatment response, tumor aggressiveness, and host survival. Activation of the coagulation cascade is related to these phenomena through molecules that interact in these processes. As such, it is necessary to identify these mediators to facilitate treatment and improve outcomes.

Publication Information

Output type

Research Output: Chapter in Book/Report/Conference proceeding Chapter

Original language

English

Pages from-to (Number of pages)

Pages 213-242 (30 pages)

Publication milestones

  • Published
    - 01/2021

Publication status

Published
- 01/2021

Volume

105

Publisher

Academic Press Inc., United States

Publication series

  • Publication series name: Advances in Clinical Chemistry
    ISSN (Print): 0065-2423
    ISSN (Electronic): 2162-9471
    Volume: 105
9780128246276

External Publication IDs

  • Scopus: 85104607478
  • PubMed: 34809828

Host publication title

Advances in Clinical Chemistry

Host publication editors

  • Gregory S. Makowski
  • Gregory S. Makowski

Funding Details

The authors state that they have no conflicts of interest; we received no extra-institutional funding.