Charles F. Morris
Amgen
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Publication
Featured researches published by Charles F. Morris.
Journal of Clinical Investigation | 1994
Thomas R. Ulich; Eunhee S. Yi; Ken Longmuir; Songmei Yin; Rebecca Biltz; Charles F. Morris; Regina M. Housley; Glenn F. Pierce
Keratinocyte growth factor (KGF) administered as a single intratracheal injection causes a prominent dose-dependent proliferation of type II alveolar epithelial cells in the lungs of adult rats. The increase in mitotically active alveolar cells histologically appears as a micropapillary epithelial cell hyperplasia after 2 d and peaks after 3 d in the form of monolayers of cuboidal epithelial cells lining alveolar septae. Proliferating cell nuclear antigen immunohistochemistry confirmed the profound proliferative response induced by KGF. The hyperplastic alveolar lining cells contain immunoreactive surfactant protein B and are ultrastructurally noted to contain lamellar inclusions characteristic of surfactant-producing type II pneumocytes. Mild focal bronchiolar epithelial hyperplasia is noted but is much less striking than the proliferation of type II pneumocytes. Large airways are unaffected by KGF. Daily intravenous injection of KGF is also able to cause pneumocyte proliferation. The normal adult rat lung constitutively expresses both KGF and KGF receptor mRNA, suggesting that endogenous KGF may be implicated in the paracrine regulation of the growth of pneumocytes. In conclusion, KGF rapidly and specifically induces proliferation and differentiation of type II pneumocytes in the normal adult lung.
Journal of Clinical Investigation | 1994
Regina M. Housley; Charles F. Morris; William J. Boyle; Brian Ring; Rebecca Biltz; John Tarpley; Sharon Lea Aukerman; Peter L. Devine; Robert H. Whitehead; Glenn F. Pierce
Keratinocyte growth factor (KGF), a member of the fibroblast growth factor (FGF) family, was identified as a specific keratinocyte mitogen after isolation from a lung fibroblast line. Recently, recombinant (r)KGF was found to influence proliferation and differentiation patterns of multiple epithelial cell lineages within skin, lung, and the reproductive tract. In the present study, we designed experiments to identify additional target tissues, and focused on the rat gastrointestinal (GI) system, since a putative receptor, K-sam, was originally identified in a gastric carcinoma. Expression of KGF receptor and KGF mRNA was detected within the entire GI tract, suggesting the gut both synthesized and responded to KGF. Therefore, rKGF was administered to adult rats and was found to induce markedly increased proliferation of epithelial cells from the foregut to the colon, and of hepatocytes, one day after systemic treatment. Daily treatment resulted in the marked selective induction of mucin-producing cell lineages throughout the GI tract in a dose-dependent fashion. Other cell lineages were either unaffected (e.g., Paneth cells), or relatively decreased (e.g., parietal cells, enterocytes) in rKGF-treated rats. The direct effect of rKGF was confirmed by demonstrating markedly increased carcinoembryonic antigen production in a human colon carcinoma cell line, LIM1899. Serum levels of albumin were specifically and significantly elevated after daily treatment. These results demonstrate rKGF can induce epithelial cell activation throughout the GI tract and liver. Further, endogenous KGF may be a normal paracrine mediator of growth within the gut.
American Journal of Pathology | 1994
Thomas R. Ulich; Eunhee S. Yi; Robert D. Cardiff; Songmei Yin; Nadim Bikhazi; Rebecca Biltz; Charles F. Morris; Glenn F. Pierce
American Journal of Pathology | 1994
Eunhee S. Yi; Songmei Yin; Donna L. Harclerode; Adriana Bedoya; Nadim Bikhazi; Regina M. Housley; Sharon L. Aukerman; Charles F. Morris; Glenn F. Pierce; Thomas R. Ulich
Biochemistry | 1999
Yueh-Rong Hsu; Rebecca Nybo; John K. Sullivan; Victoria J. Costigan; Christopher S. Spahr; Caroline Wong; Michael R. Jones; Andrea G. Pentzer; Jill Crouse; Robert E. Pacifici; Hsieng S. Lu; Charles F. Morris; John S. Philo
Archive | 1995
Glenn F. Pierce; Regina M. Housley; Charles F. Morris
Archive | 1995
Charles F. Morris; William C. Kenney; Bao-Lu Chen; Eric W Hsu
Archive | 1994
Glenn F. Pierce; Regina M. Housley; Charles F. Morris
Protein Expression and Purification | 1998
Yueh-Rong Hsu; Eric W Hsu; Viswanatham Katta; David Brankow; Julia Tseng; Sylvia Hu; Charles F. Morris; William C. Kenney; Hsieng S. Lu
Archive | 1994
Shi-Yuan Meng; Charles F. Morris; Larry B. Tsai