TY - JOUR
T1 - Loss of the anion exchanger DRA (Slc26a3), or PAT1 (slc26a6), alters sulfate transport by the distal ileum and overall sulfate homeostasis
AU - Whittamore, Jonathan M.
AU - Hatch, Marguerite
N1 - Funding Information:
This work was supported by National Institute of Diabetes and Digestive and Kidney Diseases Grants 56245, 81624, and 88892 to M. Hatch.
Publisher Copyright:
© 2017 the American Physiological Society.
PY - 2017/9
Y1 - 2017/9
N2 - The ileum is considered the primary site of inorganic sulfate (formula presented) absorption. In the present study, we explored the contributions of the apical chloride/bicarbonate (formula presented) exchangers downregulated in adenoma (DRA; Slc26a3), and putative anion transporter 1 (PAT1; Slc26a6), to the underlying transport mechanism. Transepithelial (formula presented) and36Cl- fluxes were determined across isolated, short-circuited segments of the distal ileum from wild-type (WT), DRA-knockout (KO), and PAT1-KO mice, together with measurements of urine and plasma sulfate. The WT distal ileum supported net sulfate absorption [197.37 ± 13.61 (SE) nmol·cm-2·h-1], but neither DRA nor PAT1 directly contributed to the unidirectional mucosal-to-serosal flux (formula presented), which was sensitive to serosal (but not mucosal) DIDS, dependent on Cl-, and regulated by cAMP. However, the absence of DRA significantly enhanced net sulfate absorption by one-third via a simultaneous rise in (formula presented) and a 30% reduction to the secretory serosal-to-mucosal flux (formula presented). We propose that DRA, together with PAT1, contributes to (formula presented) by mediating sulfate efflux across the apical membrane. Associated with increased ileal sulfate absorption in vitro, plasma sulfate was 61% greater, and urinary sulfate excretion (USO4) 2.2-fold higher, in DRA-KO mice compared with WT controls, whereas USO4 was increased 1.8-fold in PAT1-KO mice. These alterations to sulfate homeostasis could not be accounted for by any changes to renal sulfate handling suggesting that the source of this additional sulfate was intestinal. In summary, we characterized transepithelial sulfate fluxes across the mouse distal ileum demonstrating that DRA (and to a lesser extent, PAT1) secretes sulfate with significant implications for intestinal sulfate absorption and overall homeostasis. New & Noteworthy Sulfate is an essential anion that is actively absorbed from the small intestine involving members of the Slc26 gene family. Here, we show that the main intestinal chloride transporter Slc26a3, known as downregulated in adenoma (DRA), also handles sulfate and contributes to its secretion into the lumen. In the absence of functional DRA (as in the disease congenital chloride diarrhea), net intestinal sulfate absorption was significantly enhanced resulting in substantial alterations to overall sulfate homeostasis.
AB - The ileum is considered the primary site of inorganic sulfate (formula presented) absorption. In the present study, we explored the contributions of the apical chloride/bicarbonate (formula presented) exchangers downregulated in adenoma (DRA; Slc26a3), and putative anion transporter 1 (PAT1; Slc26a6), to the underlying transport mechanism. Transepithelial (formula presented) and36Cl- fluxes were determined across isolated, short-circuited segments of the distal ileum from wild-type (WT), DRA-knockout (KO), and PAT1-KO mice, together with measurements of urine and plasma sulfate. The WT distal ileum supported net sulfate absorption [197.37 ± 13.61 (SE) nmol·cm-2·h-1], but neither DRA nor PAT1 directly contributed to the unidirectional mucosal-to-serosal flux (formula presented), which was sensitive to serosal (but not mucosal) DIDS, dependent on Cl-, and regulated by cAMP. However, the absence of DRA significantly enhanced net sulfate absorption by one-third via a simultaneous rise in (formula presented) and a 30% reduction to the secretory serosal-to-mucosal flux (formula presented). We propose that DRA, together with PAT1, contributes to (formula presented) by mediating sulfate efflux across the apical membrane. Associated with increased ileal sulfate absorption in vitro, plasma sulfate was 61% greater, and urinary sulfate excretion (USO4) 2.2-fold higher, in DRA-KO mice compared with WT controls, whereas USO4 was increased 1.8-fold in PAT1-KO mice. These alterations to sulfate homeostasis could not be accounted for by any changes to renal sulfate handling suggesting that the source of this additional sulfate was intestinal. In summary, we characterized transepithelial sulfate fluxes across the mouse distal ileum demonstrating that DRA (and to a lesser extent, PAT1) secretes sulfate with significant implications for intestinal sulfate absorption and overall homeostasis. New & Noteworthy Sulfate is an essential anion that is actively absorbed from the small intestine involving members of the Slc26 gene family. Here, we show that the main intestinal chloride transporter Slc26a3, known as downregulated in adenoma (DRA), also handles sulfate and contributes to its secretion into the lumen. In the absence of functional DRA (as in the disease congenital chloride diarrhea), net intestinal sulfate absorption was significantly enhanced resulting in substantial alterations to overall sulfate homeostasis.
KW - Chloride secretion
KW - Downregulated in adenoma
KW - Putative anion transporter 1
KW - Slc13a1
KW - Slc26a1
KW - Ussing chamber
UR - http://www.scopus.com/inward/record.url?scp=85028764819&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85028764819&partnerID=8YFLogxK
U2 - 10.1152/ajpgi.00079.2017
DO - 10.1152/ajpgi.00079.2017
M3 - Article
C2 - 28526688
AN - SCOPUS:85028764819
SN - 0193-1857
VL - 313
SP - G166-G179
JO - American Journal of Physiology - Gastrointestinal and Liver Physiology
JF - American Journal of Physiology - Gastrointestinal and Liver Physiology
IS - 3
ER -