CD34 is expressed on the surface of hematopoietic stem/progenitor cells, stromal cells, and on the surface of high-endothelial venules (HEV). CD34 binds L-selectin, an adhesion molecule important for leukocyte rolling on venules and lymphocyte homing to peripheral lymph nodes (PLN). We generated CD34-deficient mutant animals through the use of homologous recombination. Wild-type and mutant animals showed no differences in lymphocyte binding to PLN HEV, in leukocyte rolling on venules or homing to PLN, in neutrophil extravasation into peritoneum in response to inflammatory stimulus, nor in delayed type hypersensitivity. Anti-L-selectin monoclonal antibody (MEL-14) also inhibited these immune responses similarly in both CD34-deficient and wild-type mice. However, eosinophil accumulation in the lung after inhalation of a model allergen, ovalbumin, is several-fold lower in mutant mice. We found no abnormalities in hematopoiesis in adult mice and interactions between mutant progenitor cells and a stromal cell line in vitro were normal. No differences existed in the recovery of progenitor cells after 5-fluorouracil treatment, nor in the mobilization of progenitor cells after granulocyte colony-stimulating factor treatment compared with wild-type animals. Surprisingly, although CD34 was not expressed in these mice, a portion of its 90-kD band crossreactive with MECA79 remained after Western blot. Thus, we have identified an additional molecule(s) that might be involved in leukocyte trafficking. These results indicate that CD34 plays an important role in eosinophil trafficking into the lung.
ARTICLES|
May 1, 1996
CD34-deficient mice have reduced eosinophil accumulation after allergen exposure and show a novel crossreactive 90-kD protein
A Suzuki,
A Suzuki
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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DP Andrew,
DP Andrew
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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JA Gonzalo,
JA Gonzalo
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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M Fukumoto,
M Fukumoto
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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J Spellberg,
J Spellberg
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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M Hashiyama,
M Hashiyama
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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H Takimoto,
H Takimoto
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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N Gerwin,
N Gerwin
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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I Webb,
I Webb
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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G Molineux,
G Molineux
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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R Amakawa,
R Amakawa
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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Y Tada,
Y Tada
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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A Wakeham,
A Wakeham
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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J Brown,
J Brown
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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I McNiece,
I McNiece
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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K Ley,
K Ley
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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EC Butcher,
EC Butcher
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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T Suda,
T Suda
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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JC Gutierrez-Ramos,
JC Gutierrez-Ramos
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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TW Mak
TW Mak
Amgen Institute, Ontario Cancer Institute, Department of Medical Biophysics, Toronto, Canada.
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Blood (1996) 87 (9): 3550–3562.
Citation
A Suzuki, DP Andrew, JA Gonzalo, M Fukumoto, J Spellberg, M Hashiyama, H Takimoto, N Gerwin, I Webb, G Molineux, R Amakawa, Y Tada, A Wakeham, J Brown, I McNiece, K Ley, EC Butcher, T Suda, JC Gutierrez-Ramos, TW Mak; CD34-deficient mice have reduced eosinophil accumulation after allergen exposure and show a novel crossreactive 90-kD protein. Blood 1996; 87 (9): 3550–3562. doi: https://doi.org/10.1182/blood.V87.9.3550.bloodjournal8793550
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