Allergen induced pulmonary inflammation enhances mammary tumor growth and metastasis: Role of CHI3L1

Allergen induced pulmonary inflammation enhances mammary tumor growth and metastasis: Role of CHI3L1

Pre‐existing pulmonary inflammation accelerates tumor growth and metastasis through its effects on myeloid cells and proinflammatory molecules, including CHI3L1. Metastasis is the primary cause of mortality in women with breast cancer. Metastasis to the lungs is greater in patients with pulmonary in...

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Veröffentlicht in:Journal of leukocyte biology 2015-05, Vol.97 (5), p.929-940
Hauptverfasser: Libreros, Stephania, Garcia‐Areas, Ramon, Keating, Patricia, Gazaniga, Nathalia, Robinson, Philip, Humbles, Alison, Iragavarapu‐Charyulu, Vijaya L.
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breast cancer
chitinase
lung
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container_end_page 940
container_issue 5
container_start_page 929
container_title Journal of leukocyte biology
container_volume 97
creator Libreros, Stephania
Garcia‐Areas, Ramon
Keating, Patricia
Gazaniga, Nathalia
Robinson, Philip
Humbles, Alison
Iragavarapu‐Charyulu, Vijaya L.
description Pre‐existing pulmonary inflammation accelerates tumor growth and metastasis through its effects on myeloid cells and proinflammatory molecules, including CHI3L1. Metastasis is the primary cause of mortality in women with breast cancer. Metastasis to the lungs is greater in patients with pulmonary inflammatory illnesses. It is unknown how pre‐existing pulmonary inflammation affects mammary tumor progression. We developed a novel breast cancer model in which pulmonary inflammation is induced in mice prior to tumor cell implantation. In the present study, we determined how pre‐existing allergen‐induced inflammation changes the pulmonary microenvironment to exacerbate tumor metastasis. We showed that pre‐existing pulmonary inflammation in mammary tumor bearers is associated with: 1) an increase in growth of the primary tumor and metastasis; 2) an increase in the expression of a glycoprotein known as CHI3L1; and 3) increase in the levels of myeloid populations in their lungs. We also showed that myeloid derived cells from the lungs of allergic tumor bearers produce higher amounts of CHI3L1 than the saline controls. We previously showed that CHI3L1 induces the expression of proinflammatory and protumorigenic molecules. In this study, we show that CHI3L1 knockout tumor bearers with pre‐existing allergic pulmonary inflammation had decreased levels of myeloid‐derived cells, decreased levels of proinflammatory mediators, and a significant reduction in tumor volume and metastasis compared with the wild‐type controls. Pre‐existing inflammation and CHI3L1 might be driving the establishment of a premetastatic milieu in the lungs and aiding in the support of metastatic foci. Understanding the role of allergen‐induced CHI3L1 and inflammation in tumor bearers and its effects on the pulmonary microenvironment could result in targeted therapies for breast cancer.
doi_str_mv 10.1189/jlb.3A0214-114RR
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Metastasis is the primary cause of mortality in women with breast cancer. Metastasis to the lungs is greater in patients with pulmonary inflammatory illnesses. It is unknown how pre‐existing pulmonary inflammation affects mammary tumor progression. We developed a novel breast cancer model in which pulmonary inflammation is induced in mice prior to tumor cell implantation. In the present study, we determined how pre‐existing allergen‐induced inflammation changes the pulmonary microenvironment to exacerbate tumor metastasis. We showed that pre‐existing pulmonary inflammation in mammary tumor bearers is associated with: 1) an increase in growth of the primary tumor and metastasis; 2) an increase in the expression of a glycoprotein known as CHI3L1; and 3) increase in the levels of myeloid populations in their lungs. We also showed that myeloid derived cells from the lungs of allergic tumor bearers produce higher amounts of CHI3L1 than the saline controls. We previously showed that CHI3L1 induces the expression of proinflammatory and protumorigenic molecules. In this study, we show that CHI3L1 knockout tumor bearers with pre‐existing allergic pulmonary inflammation had decreased levels of myeloid‐derived cells, decreased levels of proinflammatory mediators, and a significant reduction in tumor volume and metastasis compared with the wild‐type controls. Pre‐existing inflammation and CHI3L1 might be driving the establishment of a premetastatic milieu in the lungs and aiding in the support of metastatic foci. 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Metastasis is the primary cause of mortality in women with breast cancer. Metastasis to the lungs is greater in patients with pulmonary inflammatory illnesses. It is unknown how pre‐existing pulmonary inflammation affects mammary tumor progression. We developed a novel breast cancer model in which pulmonary inflammation is induced in mice prior to tumor cell implantation. In the present study, we determined how pre‐existing allergen‐induced inflammation changes the pulmonary microenvironment to exacerbate tumor metastasis. We showed that pre‐existing pulmonary inflammation in mammary tumor bearers is associated with: 1) an increase in growth of the primary tumor and metastasis; 2) an increase in the expression of a glycoprotein known as CHI3L1; and 3) increase in the levels of myeloid populations in their lungs. We also showed that myeloid derived cells from the lungs of allergic tumor bearers produce higher amounts of CHI3L1 than the saline controls. We previously showed that CHI3L1 induces the expression of proinflammatory and protumorigenic molecules. In this study, we show that CHI3L1 knockout tumor bearers with pre‐existing allergic pulmonary inflammation had decreased levels of myeloid‐derived cells, decreased levels of proinflammatory mediators, and a significant reduction in tumor volume and metastasis compared with the wild‐type controls. Pre‐existing inflammation and CHI3L1 might be driving the establishment of a premetastatic milieu in the lungs and aiding in the support of metastatic foci. 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subjects breast cancer
chitinase
lung
title Allergen induced pulmonary inflammation enhances mammary tumor growth and metastasis: Role of CHI3L1
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