Literature DB >> 34548396

Assembly and organization of the N-terminal region of mucin MUC5AC: Indications for structural and functional distinction from MUC5B.

Jerome Carpenter1,2, Yang Wang1,2, Richa Gupta1,2, Yuanli Li1,2, Prashamsha Haridass1,2, Durai B Subramani1, Boris Reidel1,2, Lisa Morton1, Caroline Ridley3,4, Wanda K O'Neal1, Marie-Pierre Buisine5, Camille Ehre1, David J Thornton3,4, Mehmet Kesimer6,2.   

Abstract

Elevated levels of MUC5AC, one of the major gel-forming mucins in the lungs, are closely associated with chronic obstructive lung diseases such as chronic bronchitis and asthma. It is not known, however, how the structure and/or gel-making properties of MUC5AC contribute to innate lung defense in health and drive the formation of stagnant mucus in disease. To understand this, here we studied the biophysical properties and macromolecular assembly of MUC5AC compared to MUC5B. To study each native mucin, we used Calu3 monomucin cultures that produced MUC5AC or MUC5B. To understand the macromolecular assembly of MUC5AC through N-terminal oligomerization, we expressed a recombinant whole N-terminal domain (5ACNT). Scanning electron microscopy and atomic force microscopy imaging indicated that the two mucins formed distinct networks on epithelial and experimental surfaces; MUC5B formed linear, infrequently branched multimers, whereas MUC5AC formed tightly organized networks with a high degree of branching. Quartz crystal microbalance-dissipation monitoring experiments indicated that MUC5AC bound significantly more to hydrophobic surfaces and was stiffer and more viscoelastic as compared to MUC5B. Light scattering analysis determined that 5ACNT primarily forms disulfide-linked covalent dimers and higher-order oligomers (i.e., trimers and tetramers). Selective proteolytic digestion of the central glycosylated region of the full-length molecule confirmed that MUC5AC forms dimers and higher-order oligomers through its N terminus. Collectively, the distinct N-terminal organization of MUC5AC may explain the more adhesive and unique viscoelastic properties of branched, highly networked MUC5AC gels. These properties may generate insight into why/how MUC5AC forms a static, "tethered" mucus layer in chronic muco-obstructive lung diseases.

Entities:  

Keywords:  MUC5AC; airways; lung; mucin; mucus gel

Mesh:

Substances:

Year:  2021        PMID: 34548396      PMCID: PMC8488587          DOI: 10.1073/pnas.2104490118

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  37 in total

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9.  Granule-stored MUC5B mucins are packed by the non-covalent formation of N-terminal head-to-head tetramers.

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Journal:  J Biol Chem       Date:  2018-02-13       Impact factor: 5.157

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