Spontaneous lung and lymph node metastasis in transgenic breast cancer is independent of the urokinase receptor uPAR

Almholt, Kasper; Laerum, Ole Didrik; Nielsen, Boye Schnack; Lund, Ida Katrine; Lund, Leif Roge; Romer, John; Jögi, Annika

Spontaneous lung and lymph node metastasis in transgenic breast cancer is independent of the urokinase receptor uPAR

Mark

Almholt, Kasper ; Laerum, Ole Didrik ; Nielsen, Boye Schnack ; Lund, Ida Katrine ; Lund, Leif Roge ; Romer, John and Jögi, Annika ^LU (2015) In Clinical and Experimental Metastasis 32(6). p.543-554

Abstract: Urokinase-type plasminogen activator (uPA) is an extracellular protease that plays a pivotal role in tumor progression. uPA activity is spatially restricted by its anchorage to high-affinity uPA receptors (uPAR) at the cell surface. High tumor tissue expression of uPA and uPAR is associated with poor prognosis in lung, breast, and colon cancer patients in clinical studies. Genetic deficiency of uPA leads to a significant reduction in metastases in the murine transgenic MMTV-PyMT breast cancer model, demonstrating a causal role for uPA in cancer dissemination. To investigate the role of uPAR in cancer progression, we analyze the effect of uPAR deficiency in the same cancer model. uPAR is predominantly expressed in stromal cells in the mouse... (More); Urokinase-type plasminogen activator (uPA) is an extracellular protease that plays a pivotal role in tumor progression. uPA activity is spatially restricted by its anchorage to high-affinity uPA receptors (uPAR) at the cell surface. High tumor tissue expression of uPA and uPAR is associated with poor prognosis in lung, breast, and colon cancer patients in clinical studies. Genetic deficiency of uPA leads to a significant reduction in metastases in the murine transgenic MMTV-PyMT breast cancer model, demonstrating a causal role for uPA in cancer dissemination. To investigate the role of uPAR in cancer progression, we analyze the effect of uPAR deficiency in the same cancer model. uPAR is predominantly expressed in stromal cells in the mouse primary tumors, similar to human breast cancer. In a cohort of MMTV-PyMT mice [uPAR-deficient (n = 31) or wild type controls (n = 33)], tumorigenesis, tumor growth, and tumor histopathology were not significantly affected by uPAR deficiency. Lung and lymph node metastases were also not significantly affected by uPAR deficiency, in contrast to the significant reduction seen in uPA-deficient mice. Taken together, our data show that the genetic absence of uPAR does not influence the outcome of the MMTV-PyMT cancer model. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/7773668

author

Almholt, Kasper ; Laerum, Ole Didrik ; Nielsen, Boye Schnack ; Lund, Ida Katrine ; Lund, Leif Roge ; Romer, John and Jögi, Annika ^LU

organization

publishing date

2015

type

Contribution to journal

publication status

published

subject

Cancer and Oncology

keywords

Metastasis, uPAR, Antibody, Mouse model, Breast cancer

in

Clinical and Experimental Metastasis

volume

32

issue

6

pages

543 - 554

publisher

Springer

external identifiers

wos:000358249700003
scopus:84937966777
pmid:26040548

ISSN

1573-7276

DOI

10.1007/s10585-015-9726-1

language

English

LU publication?

yes

id

4be13970-a5da-4213-8200-83fd63b2242c (old id 7773668)

date added to LUP

2016-04-01 10:02:24

date last changed

2022-03-12 01:31:58

@article{4be13970-a5da-4213-8200-83fd63b2242c,
  abstract     = {{Urokinase-type plasminogen activator (uPA) is an extracellular protease that plays a pivotal role in tumor progression. uPA activity is spatially restricted by its anchorage to high-affinity uPA receptors (uPAR) at the cell surface. High tumor tissue expression of uPA and uPAR is associated with poor prognosis in lung, breast, and colon cancer patients in clinical studies. Genetic deficiency of uPA leads to a significant reduction in metastases in the murine transgenic MMTV-PyMT breast cancer model, demonstrating a causal role for uPA in cancer dissemination. To investigate the role of uPAR in cancer progression, we analyze the effect of uPAR deficiency in the same cancer model. uPAR is predominantly expressed in stromal cells in the mouse primary tumors, similar to human breast cancer. In a cohort of MMTV-PyMT mice [uPAR-deficient (n = 31) or wild type controls (n = 33)], tumorigenesis, tumor growth, and tumor histopathology were not significantly affected by uPAR deficiency. Lung and lymph node metastases were also not significantly affected by uPAR deficiency, in contrast to the significant reduction seen in uPA-deficient mice. Taken together, our data show that the genetic absence of uPAR does not influence the outcome of the MMTV-PyMT cancer model.}},
  author       = {{Almholt, Kasper and Laerum, Ole Didrik and Nielsen, Boye Schnack and Lund, Ida Katrine and Lund, Leif Roge and Romer, John and Jögi, Annika}},
  issn         = {{1573-7276}},
  keywords     = {{Metastasis; uPAR; Antibody; Mouse model; Breast cancer}},
  language     = {{eng}},
  number       = {{6}},
  pages        = {{543--554}},
  publisher    = {{Springer}},
  series       = {{Clinical and Experimental Metastasis}},
  title        = {{Spontaneous lung and lymph node metastasis in transgenic breast cancer is independent of the urokinase receptor uPAR}},
  url          = {{http://dx.doi.org/10.1007/s10585-015-9726-1}},
  doi          = {{10.1007/s10585-015-9726-1}},
  volume       = {{32}},
  year         = {{2015}},
}

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Spontaneous lung and lymph node metastasis in transgenic breast cancer is independent of the urokinase receptor uPAR