Transforming growth factor-beta (TGF-beta) is secreted in a latent form and activated during co-culture of endothelial cells and smooth muscle cells. Plasmin located on the surface of endothelial cells is required for the activation of latent TGF-beta (LTGF-beta) during co-culture, and the targeting of LTGF-beta to the cellular surface is requisite for its activation. In the present study, the cellular targeting of LTGF-beta was examined. We detected the specific binding of 125I-large LTGF-beta 1 isolated from human platelets to smooth muscle cells but not to endothelial cells. A mAb against the latency-associated peptide (LAP) of large LTGF-beta 1 complex, which blocked the binding of 125I-large LTGF-beta 1 to smooth muscle cells, inhibited the activation of LTGF-beta during co-culture. The binding of 125I-large LTGF-beta 1 could not be competed either by mannose-6-phosphate (300 microM) or by the synthetic peptide Arg-Gly-Asp-Ser (300 micrograms/ml). These results indicate that the targeting of LTGF-beta to smooth muscle cells is required for the activation of LTGF-beta during co-culture of endothelial cells and smooth muscle cells. The targeting of LTGF-beta to smooth muscle cells is mediated by LAP, and the domain of LAP responsible for the targeting to smooth muscle cells may not be related to mannose-6-phosphate or an Arg-Gly-Asp sequence, both of which have been previously proposed as candidates for the cellular binding domains within LAP.
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1 December 1993
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December 01 1993
The mechanism for the activation of latent TGF-beta during co-culture of endothelial cells and smooth muscle cells: cell-type specific targeting of latent TGF-beta to smooth muscle cells.
Y Sato,
Y Sato
Department of Internal Medicine 1, Oita Medical University, Japan.
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F Okada,
F Okada
Department of Internal Medicine 1, Oita Medical University, Japan.
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M Abe,
M Abe
Department of Internal Medicine 1, Oita Medical University, Japan.
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T Seguchi,
T Seguchi
Department of Internal Medicine 1, Oita Medical University, Japan.
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M Kuwano,
M Kuwano
Department of Internal Medicine 1, Oita Medical University, Japan.
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S Sato,
S Sato
Department of Internal Medicine 1, Oita Medical University, Japan.
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A Furuya,
A Furuya
Department of Internal Medicine 1, Oita Medical University, Japan.
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N Hanai,
N Hanai
Department of Internal Medicine 1, Oita Medical University, Japan.
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T Tamaoki
T Tamaoki
Department of Internal Medicine 1, Oita Medical University, Japan.
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Y Sato
Department of Internal Medicine 1, Oita Medical University, Japan.
F Okada
Department of Internal Medicine 1, Oita Medical University, Japan.
M Abe
Department of Internal Medicine 1, Oita Medical University, Japan.
T Seguchi
Department of Internal Medicine 1, Oita Medical University, Japan.
M Kuwano
Department of Internal Medicine 1, Oita Medical University, Japan.
S Sato
Department of Internal Medicine 1, Oita Medical University, Japan.
A Furuya
Department of Internal Medicine 1, Oita Medical University, Japan.
N Hanai
Department of Internal Medicine 1, Oita Medical University, Japan.
T Tamaoki
Department of Internal Medicine 1, Oita Medical University, Japan.
Online ISSN: 1540-8140
Print ISSN: 0021-9525
J Cell Biol (1993) 123 (5): 1249–1254.
Citation
Y Sato, F Okada, M Abe, T Seguchi, M Kuwano, S Sato, A Furuya, N Hanai, T Tamaoki; The mechanism for the activation of latent TGF-beta during co-culture of endothelial cells and smooth muscle cells: cell-type specific targeting of latent TGF-beta to smooth muscle cells.. J Cell Biol 1 December 1993; 123 (5): 1249–1254. doi: https://doi.org/10.1083/jcb.123.5.1249
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