Pii: S0003-9969(01)00027-9
نویسندگان
چکیده
Late-gestation (embryonic day 18; E18) mouse submandibular glands (SMG) comprise a network of large and small ducts that terminate in lumen-containing, presumptive acini (terminal buds) expressing unique, cell membraneassociated embryonic mucin. The objective here was to clone and sequence embryonic low molecular-weight SMG mucin, predict its secondary structure, and begin to investigate its possible role in SMG development. Evidence was found that: (1) embryonic low molecular-weight mucin is an alternatively spliced Muc10 gene product, 220 amino acids in size (approximately 25 kDa), rich in potential O-glycosylation sites, and variably glycosylated (approximately 40 and 68 kDa); (2) consensus secondary-structure prediction for embryonic low molecular-weight mucin is consistent with a molecule that is anchored to the plasma membrane, directly or indirectly (via a glycolipid), and has a protein core that serves as a scaffold for carbohydrate presentation; (3) embryonic L-selectin is immunolocalized to the plasma membrane region of terminal-bud epithelial cells in a pattern similar to that seen for embryonic mucin; (4) embryonic, but not adult, mucin is able to bind L-selectin and does so endogenously in E18 SMG. As the primary role of L-selectin is to mediate cell adhesion and its ligands are mucin-like glycoproteins, it is suggested that this embryonic low molecular-weight mucin be termed MucCAM. © 2001 Elsevier Science Ltd. All rights reserved.
منابع مشابه
Pii: S0003-9969(96)00027-1
J. CARLESON, 1'2 P. ALSTERGREN, 2 A. APPELGREN, 2 B. APPELGREN, 2 S. KOPP, 2 G. R. SRINIVASAN, 4 E. THEODORSSON 4 and T. LUNDEBERG 1'3'* ~Department of Physiology and Pharmacology, Division of Physiology II, S-171 77, Stockholm, Sweden, 2Center for Clinical Oral Science, School of Dentistry, Karolinska Institutet, Box 4064, S-141 04, Huddinge, Sweden, 3Nociceptive Pain Unit, Department of Rehab...
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