2016
DOI: 10.1096/fj.201600223r
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Inhibitors of pendrin anion exchange identified in a small molecule screen increase airway surface liquid volume in cystic fibrosis

Abstract: Pendrin (SLC26A4) is a Cl 2 /anion exchanger expressed in the epithelium of inflamed airways where it is thought to facilitate Cl 2 absorption and HCO 3 2 secretion. Studies using pendrin knockout mice and airway epithelial cells from hearing-impaired subjects with pendrin loss of function suggest involvement of pendrin in inflammatory lung diseases, including cystic fibrosis (CF), perhaps by regulation of airway surface liquid (ASL) volume. Here we identified small-molecule pendrin inhibitors and demonstrated… Show more

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Cited by 52 publications
(72 citation statements)
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References 71 publications
(125 reference statements)
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“…FRT epithelial cells (UCSF Cell Culture Facility), HEK cells (UCSF Cell Culture Facility), and HBE cell cultures (UCSF Cystic Fibrosis Research Development Program) were cultured using standard methods (19). For slc26a3 inhibitor screening, an FRT cell line virally transduced to express YFP (46) was transfected with pIRESpuro3-slc26a3, selected using 0.15 μg/ml puromycin, and a clonal cell line (termed FRT-YFP-slc26a3) was isolated.…”
Section: Methodsmentioning
confidence: 99%
See 1 more Smart Citation
“…FRT epithelial cells (UCSF Cell Culture Facility), HEK cells (UCSF Cell Culture Facility), and HBE cell cultures (UCSF Cystic Fibrosis Research Development Program) were cultured using standard methods (19). For slc26a3 inhibitor screening, an FRT cell line virally transduced to express YFP (46) was transfected with pIRESpuro3-slc26a3, selected using 0.15 μg/ml puromycin, and a clonal cell line (termed FRT-YFP-slc26a3) was isolated.…”
Section: Methodsmentioning
confidence: 99%
“…The closest SLC26A3 homolog, SLC26A4 (pendrin; 45% amino acid identity), is an anion exchanger in the inner ear, thyroid, inflamed airways, and kidney (6,9,18). We previously identified small-molecule pendrin inhibitors that increased airway surface liquid depth in airway epithelial cell cultures and produced a diuretic response in mice, suggesting potential therapeutic utility in inflammatory lung disorders, such as CF and asthma, and in volume-overload edema (19,20). The second most closely related SLC26A3 homolog, SLC26A6 (putative anion transporter-1 [PAT-1]; 34% amino acid identity), is also an anion exchanger expressed at the apical membrane in the small intestine that, together with SLC26A3, facilitates electroneutral NaCl absorption (21,22).…”
Section: Introductionmentioning
confidence: 99%
“…Amiloride-sensitive ENaC activity was measured by short-circuit current analysis of human bronchial epithelial cell cultures. 13 Specificity assays were done with 25 mM PDS inh -C01. …”
Section: Cell Culturementioning
confidence: 99%
“…The inhibitors were identified in a high-throughput screen against human pendrin, which was recently reported. 13 Here, compounds were characterized and optimized for inhibition of murine pendrin and were tested in mice alone and in combination with short-or long-term diuretic therapy. Although no effect of pendrin inhibition alone was seen, as predicted from data in pendrin knockout mice and humans with Pendred syndrome, we found significant potentiation of the diuretic response to furosemide.…”
mentioning
confidence: 99%
“…Verkman and colleagues 14 identified novel compounds selectively inhibiting pendrin with high affinity using a functional chemical library screen. As reported here in this issue of the Journal of the American Society of Nephrology, these compounds given to mice had, per se, no effect on diuresis or acid-base parameters in urine and blood.…”
Section: /Hmentioning
confidence: 99%