Cystic fibrosis and the relationship between mucin and chloride secretion by cultures of human airway gland mucous cells

Author:

Finkbeiner Walter E.1,Zlock Lorna T.1,Morikawa Masatoshi1,Lao Anna Y.1,Dasari Vijay1,Widdicombe Jonathan H.2

Affiliation:

1. Department of Pathology, University of California, San Francisco;

2. Department of Human Physiology, University of California, Davis, California

Abstract

—We investigated how cystic fibrosis (CF) alters the relationship between Cland mucin secretion in cultures of non-CF and CF human tracheobronchial gland mucous (HTGM and CFTGM, respectively) cells. Biochemical studies showed that HTMG cells secreted typical airway mucins, and immunohistochemical studies showed that these cells expressed MUC1, MUC4, MUC5B, MUC8, MUC13, MUC16, and MUC20. Effects of cumulative doses of methacholine (MCh), phenylephrine (Phe), isoproterenol (Iso), and ATP on mucin and Clsecretion were studied on HTGM and CFTGM cultures. Baseline mucin secretion was not significantly altered in CFTGM cells, and the increases in mucin secretion induced by mediators were unaltered (Iso, Phe) or slightly decreased (MCh, ATP). Across mediators, there was no correlation between the maximal increases in Clsecretion and mucin secretion. In HTGM cells, the Clchannel blocker, diphenylamine-2-carboxylic acid, greatly inhibited Clsecretion but did not alter mucin release. In HTGM cells, mediators (10−5M) increased mucin secretion in the rank order ATP > Phe = Iso > MCh. They increased Clsecretion in the sequence ATP > MCh ≈ Iso > Phe. The responses in Clsecretion to MCh, ATP, and Phe were unaltered by CF, but the response to Iso was greatly reduced. We conclude that mucin secretion by cultures of human tracheobronchial gland cells is independent of Clsecretion, at baseline, and is unaltered in CF; that the ratio of Clsecretion to mucus secretion varies markedly depending on mediator; and that secretions induced by stimulation of β-adrenergic receptors will be abnormally concentrated in CF.

Publisher

American Physiological Society

Subject

Cell Biology,Physiology (medical),Pulmonary and Respiratory Medicine,Physiology

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