Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements

BACKGROUND: Spontaneous Regression/Complete Resistant (SR/CR) mice are a colony of cancer-resistant mice that can detect and rapidly destroy malignant cells with innate cellular immunity, predominately mediated by granulocytes. Our previous studies suggest that several effector mechanisms, such as p...

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Autores principales: Sanders, Anne M, Stehle, John R, Blanks, Michael J, Riedlinger, Gregory, Kim-Shapiro, Jung W, Monjazeb, Arta M, Adams, Jonathan M, Willingham, Mark C, Cui, Zheng
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2861034/
https://www.ncbi.nlm.nih.gov/pubmed/20356394
http://dx.doi.org/10.1186/1471-2407-10-121
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author Sanders, Anne M
Stehle, John R
Blanks, Michael J
Riedlinger, Gregory
Kim-Shapiro, Jung W
Monjazeb, Arta M
Adams, Jonathan M
Willingham, Mark C
Cui, Zheng
author_facet Sanders, Anne M
Stehle, John R
Blanks, Michael J
Riedlinger, Gregory
Kim-Shapiro, Jung W
Monjazeb, Arta M
Adams, Jonathan M
Willingham, Mark C
Cui, Zheng
author_sort Sanders, Anne M
collection PubMed
description BACKGROUND: Spontaneous Regression/Complete Resistant (SR/CR) mice are a colony of cancer-resistant mice that can detect and rapidly destroy malignant cells with innate cellular immunity, predominately mediated by granulocytes. Our previous studies suggest that several effector mechanisms, such as perforin, granzymes, or complements, may be involved in the killing of cancer cells. However, none of these effector mechanisms is known as critical for granulocytes. Additionally, it is unclear which effector mechanisms are required for the cancer killing activity of specific leukocyte populations and the survival of SR/CR mice against the challenges of lethal cancer cells. We hypothesized that if any of these effector mechanisms was required for the resistance to cancer cells, its functional knockout in SR/CR mice should render them sensitive to cancer challenges. This was tested by cross breeding SR/CR mice into the individual genetic knockout backgrounds of perforin (Prf(-/-)), superoxide (Cybb(-/)), or inducible nitric oxide (Nos2(-/)). METHODS: SR/CR mice were bred into individual Prf(-/-), Cybb(-/-), or Nos2(-/- )genetic backgrounds and then challenged with sarcoma 180 (S180). Their overall survival was compared to controls. The cancer killing efficiency of purified populations of macrophages and neutrophils from these immunodeficient mice was also examined. RESULTS: When these genetically engineered mice were challenged with cancer cells, the knockout backgrounds of Prf(-/-), Cybb(-/-), or Nos2(-/- )did not completely abolish the SR/CR cancer resistant phenotype. However, the Nos2(-/- )background did appear to weaken the resistance. Incidentally, it was also observed that the male mice in these immunocompromised backgrounds tended to be less cancer-resistant than SR/CR controls. CONCLUSION: Despite the previously known roles of perforin, superoxide or nitric oxide in the effector mechanisms of innate immune responses, these effector mechanisms were not required for cancer-resistance in SR/CR mice. The resistance was functional when any one of these effector mechanisms was completely absent, except some noticeably reduced penetrance, but not abolishment, of the phenotype in the male background in comparison to female background. These results also indicate that some other effector mechanism(s) of granulocytes may be involved in the killing of cancer cells in SR/CR mice.
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spelling pubmed-28610342010-04-29 Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements Sanders, Anne M Stehle, John R Blanks, Michael J Riedlinger, Gregory Kim-Shapiro, Jung W Monjazeb, Arta M Adams, Jonathan M Willingham, Mark C Cui, Zheng BMC Cancer Research Article BACKGROUND: Spontaneous Regression/Complete Resistant (SR/CR) mice are a colony of cancer-resistant mice that can detect and rapidly destroy malignant cells with innate cellular immunity, predominately mediated by granulocytes. Our previous studies suggest that several effector mechanisms, such as perforin, granzymes, or complements, may be involved in the killing of cancer cells. However, none of these effector mechanisms is known as critical for granulocytes. Additionally, it is unclear which effector mechanisms are required for the cancer killing activity of specific leukocyte populations and the survival of SR/CR mice against the challenges of lethal cancer cells. We hypothesized that if any of these effector mechanisms was required for the resistance to cancer cells, its functional knockout in SR/CR mice should render them sensitive to cancer challenges. This was tested by cross breeding SR/CR mice into the individual genetic knockout backgrounds of perforin (Prf(-/-)), superoxide (Cybb(-/)), or inducible nitric oxide (Nos2(-/)). METHODS: SR/CR mice were bred into individual Prf(-/-), Cybb(-/-), or Nos2(-/- )genetic backgrounds and then challenged with sarcoma 180 (S180). Their overall survival was compared to controls. The cancer killing efficiency of purified populations of macrophages and neutrophils from these immunodeficient mice was also examined. RESULTS: When these genetically engineered mice were challenged with cancer cells, the knockout backgrounds of Prf(-/-), Cybb(-/-), or Nos2(-/- )did not completely abolish the SR/CR cancer resistant phenotype. However, the Nos2(-/- )background did appear to weaken the resistance. Incidentally, it was also observed that the male mice in these immunocompromised backgrounds tended to be less cancer-resistant than SR/CR controls. CONCLUSION: Despite the previously known roles of perforin, superoxide or nitric oxide in the effector mechanisms of innate immune responses, these effector mechanisms were not required for cancer-resistance in SR/CR mice. The resistance was functional when any one of these effector mechanisms was completely absent, except some noticeably reduced penetrance, but not abolishment, of the phenotype in the male background in comparison to female background. These results also indicate that some other effector mechanism(s) of granulocytes may be involved in the killing of cancer cells in SR/CR mice. BioMed Central 2010-03-31 /pmc/articles/PMC2861034/ /pubmed/20356394 http://dx.doi.org/10.1186/1471-2407-10-121 Text en Copyright ©2010 Sanders et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Sanders, Anne M
Stehle, John R
Blanks, Michael J
Riedlinger, Gregory
Kim-Shapiro, Jung W
Monjazeb, Arta M
Adams, Jonathan M
Willingham, Mark C
Cui, Zheng
Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title_full Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title_fullStr Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title_full_unstemmed Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title_short Cancer resistance of SR/CR mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
title_sort cancer resistance of sr/cr mice in the genetic knockout backgrounds of leukocyte effector mechanisms: determinations for functional requirements
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2861034/
https://www.ncbi.nlm.nih.gov/pubmed/20356394
http://dx.doi.org/10.1186/1471-2407-10-121
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