Sodium-glucose transport proteins explained

Sodium-dependent glucose cotransporters (or sodium-glucose linked transporter, SGLT) are a family of glucose transporter found in the intestinal mucosa (enterocytes) of the small intestine (SGLT1) and the proximal tubule of the nephron (SGLT2 in PCT and SGLT1 in PST). They contribute to renal glucose reabsorption. In the kidneys, 100% of the filtered glucose in the glomerulus has to be reabsorbed along the nephron (98% in PCT, via SGLT2). If the plasma glucose concentration is too high (hyperglycemia), glucose passes into the urine (glucosuria) because SGLT are saturated with the filtered glucose.

Types

The sodium-glucose linked transporters (SGLTs) are responsible for the active transport of glucose across cell membranes. SGLT1 and SGLT2 are the most well-studied members of this family.^{[1] [2]} Both SGLT1 and SGLT2 function as symporters, utilizing the energy from the sodium gradient created by the Na+/K+ ATPase to transport glucose against its concentration gradient.

SGLT2, encoded by the SLC5A2 gene, is predominantly expressed in the S1 and S2 segments of the proximal renal tubule and is responsible for approximately 97% of glucose reabsorption in the kidneys under normal conditions. SGLT1, encoded by the SLC5A1 gene, is primarily expressed in the late proximal tubule (S3 segment) and accounts for the remaining 3% of glucose reabsorption.

In addition to SGLT1 and SGLT2, there are 10 other members in the human protein family SLC5A.^[3]

SLC5A4, also known as SGLT3, is a member of the sodium-glucose cotransporter family. Unlike SGLT1 and SGLT2, which are efficient glucose transporters, SGLT3 functions primarily as a glucose sensor rather than a transporter. It has a low affinity for glucose and does not significantly contribute to glucose transport across cell membranes. Instead, SGLT3 acts as a glucose-gated ion channel, generating small depolarizing currents in response to extracellular glucose. This electrical signaling function suggests a role in glucose sensing and signaling pathways rather than in glucose transport.^{[4] [5]}

Gene	Protein	Acronym	Tissue distribution in proximal tubule[6]	Na+:Glucose Co-transport ratio	Contribution to glucose reabsorption (%)[7]	-	SLC5A1	Sodium/GLucose coTransporter 1	SGLT1	S3 segment	2:1	10	-	SLC5A2	Sodium/GLucose coTransporter 2	SGLT2	predominantly in the S1 and S2 segments	1:1	90

The SLC5 family includes transporters for a diverse range of substrates beyond glucose. Specific members of this family are specialized for the transport of:

• Mannose (SLC5A9, also known as SGLT4)
• Myo-inositol (SLC5A3, also known as SMIT1)
• Choline (SLC5A7, also known as CHT1)
• Iodide (SLC5A5, also known as NIS)
• Vitamins, specifically biotin and pantothenate (SLC5A6, also known as SMVT)
• Short-chain fatty acids (SLC5A8 and SLC5A12, also known as SMCT1 and SMCT2 respectively)

Each of these transporters plays a specific role in cellular metabolism and homeostasis, often utilizing sodium gradients for substrate transport similar to the glucose transporters in this family.^{[8] [5]}

Mechanism

The transport of glucose across the proximal tubule cell membrane involves a complex process of secondary active transport (also known as co-transport). This process begins with the Na⁺/K⁺ ATPase on the basolateral membrane. This enzyme uses ATP to pump 3 sodium ions out of the cell into the blood while bringing 2 potassium ions into the cell.^[9] This action creates a sodium concentration gradient across the cell membrane, with a lower concentration inside the cell compared to both the blood and the tubular lumen.

SGLT proteins utilize this sodium gradient to transport glucose across the apical membrane into the cell, even against the glucose concentration gradient.^{[10] [11]} This mechanism is an example of secondary active transport. Once inside the cell, glucose is then moved across the basolateral membrane into the peritubular capillaries by members of the GLUT family of glucose uniporters.

SGLT1 and SGLT2 are classified as symporters because they move sodium and glucose in the same direction across the membrane. To maintain this process, the Sodium–hydrogen antiporter plays a crucial role in replenishing intracellular sodium levels.^{[12] [13]} Consequently, the net effect of glucose transport is coupled with the extrusion of protons from the cell, with sodium serving as an intermediate in this process.

SGLT2 inhibitors for diabetes

See main article: Gliflozin. SGLT2 inhibitors, also called gliflozins,^[14] are used in the treatment of type 2 diabetes. SGLT2 is only found in kidney tubules and in conjunction with SGLT1 resorbs glucose into the blood from the forming urine. By inhibiting SGLT2, and not targeting SGLT1, glucose is excreted which in turn lowers blood glucose levels. Examples include dapagliflozin (Farxiga in US, Forxiga in EU), canagliflozin (Invokana) and empagliflozin (Jardiance). Certain SGLT2 inhibitors have shown to reduce mortality in type 2 diabetes.^[15] The safety and efficacy of SGLT2 inhibitors have not been established in patients with type 1 diabetes, and FDA has not approved them for use in these patients.^[16]

History

In August 1960, in Prague, Robert K. Crane presented for the first time his discovery of the sodium-glucose cotransport as the mechanism for intestinal glucose absorption.^[17]

Crane's discovery of cotransport was the first-ever proposal of flux coupling in biology.^{[18] [19]}

See also

• Cotransport
• Cotransporter
• Glucose-galactose malabsorption
• Renal sodium reabsorption
• Discovery and development of SGLT-2 inhibitors

Notes and References

1. Thorens B, Mueckler M . Glucose transporters in the 21st Century . American Journal of Physiology. Endocrinology and Metabolism . 298 . 2 . E141–5 . February 2010 . 20009031 . 2822486 . 10.1152/ajpendo.00712.2009 . review .
2. Dominguez Rieg JA, Xue J, Rieg T . Tubular effects of sodium-glucose cotransporter 2 inhibitors: intended and unintended consequences . Current Opinion in Nephrology and Hypertension . 29 . 5 . 523–530 . September 2020 . 32701600. 8772383 . 10.1097/MNH.0000000000000632 . review .
3. http://www.ensembl.org/Homo_sapiens/familyview?family=ENSF00000000509 Ensembl release 48: Homo sapiens Ensembl protein family ENSF00000000509
4. Diez-Sampedro A, Hirayama BA, Osswald C, Gorboulev V, Baumgarten K, Volk C, Wright EM, Koepsell H . A glucose sensor hiding in a family of transporters . Proceedings of the National Academy of Sciences of the United States of America . 100 . 20 . 11753–8 . September 2003 . 13130073 . 208830 . 10.1073/pnas.1733027100 . free . 2003PNAS..10011753D . primary .
5. Gyimesi G, Pujol-Giménez J, Kanai Y, Hediger MA . Sodium-coupled glucose transport, the SLC5 family, and therapeutically relevant inhibitors: from molecular discovery to clinical application . Pflügers Archiv . 472 . 9 . 1177–1206 . September 2020 . 32767111 . 7462921 . 10.1007/s00424-020-02433-x . free .
6. Wright EM, Hirayama BA, Loo DF . Active sugar transport in health and disease . Journal of Internal Medicine . 261 . 1 . 32–43 . January 2007 . 17222166 . 10.1111/j.1365-2796.2006.01746.x . 44399123 .
7. Wright EM . Renal Na(+)-glucose cotransporters . American Journal of Physiology. Renal Physiology . 280 . 1 . F10–8 . January 2001 . 11133510 . 10.1152/ajprenal.2001.280.1.F10 .
8. Wright EM, Loo DD, Hirayama BA . Biology of human sodium glucose transporters . Physiological Reviews . 91 . 2 . 733–94 . April 2011 . 21527736 . 10.1152/physrev.00055.2009 . review .
9. Vallon V . Glucose transporters in the kidney in health and disease . Pflügers Archiv: European Journal of Physiology . 472 . 9 . 1345–1370 . September 2020 . 32144488 . 7483786 . 10.1007/s00424-020-02361-w . review .
10. Mudaliar S, Polidori D, Zambrowicz B, Henry RR . Sodium-Glucose Cotransporter Inhibitors: Effects on Renal and Intestinal Glucose Transport: From Bench to Bedside . Diabetes Care . 38 . 12 . 2344–53 . December 2015 . 26604280 . 10.2337/dc15-0642 . review .
11. Hotait ZS, Lo Cascio JN, Choos EN, Shepard BD . The sugar daddy: the role of the renal proximal tubule in glucose homeostasis . American Journal of Physiology. Cell Physiology . 323 . 3 . C791–C803 . September 2022 . 35912988 . 9448277 . 10.1152/ajpcell.00225.2022 . review .
12. Nwia SM, Li XC, Leite AP, Hassan R, Zhuo JL . The Na+/H+ Exchanger 3 in the Intestines and the Proximal Tubule of the Kidney: Localization, Physiological Function, and Key Roles in Angiotensin II-Induced Hypertension . Frontiers in Physiology . 13 . 861659 . 2022 . 35514347 . 9062697 . 10.3389/fphys.2022.861659 . free . review .
13. Liu J, Tian J, Sodhi K, Shapiro JI . The Na/K-ATPase Signaling and SGLT2 Inhibitor-Mediated Cardiorenal Protection: A Crossed Road? . The Journal of Membrane Biology . 254 . 5–6 . 513–529 . December 2021 . 34297135 . 10.1007/s00232-021-00192-z . 8595165 . review .
14. Web site: SGLT2 Inhibitors (Gliflozins). Diabetes.co.uk. 2015-05-19.
15. Zinman B, Wanner C, Lachin JM, Fitchett D, Bluhmki E, Hantel S, Mattheus M, Devins T, Johansen OE, Woerle HJ, Broedl UC, Inzucchi SE . Empagliflozin, Cardiovascular Outcomes, and Mortality in Type 2 Diabetes . The New England Journal of Medicine . 373 . 22 . 2117–28 . November 2015 . 26378978 . 10.1056/NEJMoa1504720 . 11573/894529 . 205098095 . free .
16. Web site: Center for Drug Evaluation and Research (CDER) . 2018-12-28. Sodium-glucose Cotransporter-2 (SGLT2) Inhibitors. U.S. Food and Drug Administration (FDA) . en.
17. Book: Crane RK, Miller D, Bihler I . The restrictions on possible mechanisms of intestinal transport of sugars . Membrane Transport and Metabolism. Proceedings of a Symposium held in Prague, August 22–27, 1960. Kleinzeller A, Kotyk A . Czech Academy of Sciences & Academic Press . 439–449 . 1961 .
18. Wright EM, Turk E . The sodium/glucose cotransport family SLC5 . Pflügers Archiv . 447 . 5 . 510–8 . February 2004 . 12748858 . 10.1007/s00424-003-1063-6 . 41985805 . Crane in 1961 was the first to formulate the cotransport concept to explain active transport [7]. Specifically, he proposed that the accumulation of glucose in the intestinal epithelium across the brush border membrane was [is] coupled to downhill Na+ transport cross the brush border. This hypothesis was rapidly tested, refined, and extended [to] encompass the active transport of a diverse range of molecules and ions into virtually every cell type. .
19. Boyd CA . Facts, fantasies and fun in epithelial physiology . Experimental Physiology . 93 . 3 . 303–14 . March 2008 . 18192340 . 10.1113/expphysiol.2007.037523 . 41086034 . p. 304. "the insight from this time that remains in all current text books is the notion of Robert Crane published originally as an appendix to a symposium paper published in 1960 (Crane et al. 1960). The key point here was 'flux coupling', the cotransport of sodium and glucose in the apical membrane of the small intestinal epithelial cell. Half a century later this idea has turned into one of the most studied of all transporter proteins (SGLT1), the sodium–glucose cotransporter. . free .