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Research ArticleExperimental Studies

Reduced Irradiation Pulmonary Fibrosis and Stromal Cell Migration in Smad3-/- Marrow Chimeric Mice

MICHAEL W. EPPERLY, DARCY FRANICOLA, XICHEN ZHANG, SUHUA NIE, HONG WANG, ALFRED B. BAHNSON, DONNA S. SHIELDS, JULIE P. GOFF, HONGMEI SHEN and JOEL S. GREENBERGER
In Vivo September 2006, 20 (5) 573-582;
MICHAEL W. EPPERLY
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DARCY FRANICOLA
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XICHEN ZHANG
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SUHUA NIE
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HONG WANG
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ALFRED B. BAHNSON
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DONNA S. SHIELDS
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JULIE P. GOFF
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HONGMEI SHEN
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JOEL S. GREENBERGER
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  • For correspondence: greenbergerjs{at}upmc.edu
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Abstract

Pulmonary irradiation fibrosis involves migration to the lungs of bone marrow origin myofibroblast progenitor cells (marrow stromal cells (MSCs)). Smad3-/- mice display decreased ionizing irradiation-induced skin fibrosis, defective osteochondrogenesis and other abnormalities thought to be associated with a defective stromal cell response(s) to transforming growth factor-beta (TGFβ). Clonal bone marrow stromal cell lines were derived from the adherent layer of continuous bone marrow cultures of homozygous deletion recombinant negative Smad3-/- mice and Smad3+/+ littermates. Quantitation in an Automated Cell Tracking System of the in vitro single cell migratory capacity over five days demonstrated a significant decrease in locomotion in microns per 24 h of Smad3-/- compared to Smad3+/+ clonal MSC lines. Reexpression by retroviral vector transfection of the Smad3 but not control ds-red transgene restored in vitro migratory capacity. Intravenously injected GFP transgene product labeled Smad3-/- (MSCs) seeded 10-fold less effectively than ds-red transgene product labeled Smad3+/+ cells to the 80 days post 20 Gy irradiated lungs of C57BL/6J mice and proliferated less significantly for 60 days after cell injection. Female mice chimeric for male Smad3-/- compared to Smad3+/+ marrow showed decreased irradiation pulmonary fibrosis, Y+ stromal cell migration to the lungs, and improved survival. The data show that the reduced in vitro and in vivo migratory capacity of Smad3-/- bone marrow stromal cells correlates with decreased radiation pulmonary fibrosis observed in mice chimeric for Smad3-/- marrow.

  • Bone marrow stromal cells
  • hematopoietic microenvironment
  • Smad3
  • TGFβ signal transduction
  • gene transfer

Footnotes

  • Received July 3, 2006.
  • Accepted July 12, 2006.
  • Copyright © 2006 The Author(s). Published by the International Institute of Anticancer Research.
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September-October 2006
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Reduced Irradiation Pulmonary Fibrosis and Stromal Cell Migration in Smad3-/- Marrow Chimeric Mice
MICHAEL W. EPPERLY, DARCY FRANICOLA, XICHEN ZHANG, SUHUA NIE, HONG WANG, ALFRED B. BAHNSON, DONNA S. SHIELDS, JULIE P. GOFF, HONGMEI SHEN, JOEL S. GREENBERGER
In Vivo Sep 2006, 20 (5) 573-582;

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Reduced Irradiation Pulmonary Fibrosis and Stromal Cell Migration in Smad3-/- Marrow Chimeric Mice
MICHAEL W. EPPERLY, DARCY FRANICOLA, XICHEN ZHANG, SUHUA NIE, HONG WANG, ALFRED B. BAHNSON, DONNA S. SHIELDS, JULIE P. GOFF, HONGMEI SHEN, JOEL S. GREENBERGER
In Vivo Sep 2006, 20 (5) 573-582;
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