Your search keyword '"Hirayama, Bruce A."' showing total 7 results

1. Fingerprints of hSGLT5 sugar and cation selectivity.

Author

Ghezzi, Chiara, Gorraitz, Edurne, Hirayama, Bruce A., Loo, Donald D. F., Grempler, Rolf, Mayoux, Eric, and Wright, Ernest M.

Subjects

SODIUM-glucose cotransporters, CHROMOSOMAL translocation, CARBOHYDRATE metabolism, MANNOSE, KNOCKOUT mice, PHLORIZIN

Abstract

Sodium glucose cotransporters (SGLTs) mediate the translocation of carbohydrates across the brush border membrane of different organs such as intestine, kidney, and brain. The human SGLT5 (hSGLT5), in particular, is localized in the kidney were it is responsible for mannose and fructose reabsorption from the glomerular filtrate as confirmed by more recent studies on hSGLT5 knockout mice. Here we characterize the functional properties of hSGLT5 expressed in a stable T-Rex- HEK-293 cell line using biochemical and electrophysiological assays. We confirmed that hSGLT5 is a sodium/mannose transporter that is blocked by phlorizin. Li+ and H+ ions were also able to drive mannose transport, and transport was electrogenic. Our results moreover indicate that substrates require a pyranose ring with an axial hydroxyl group (-OH) on carbon 2 (C-2). Compared with Na+/glucose cotransport, the level of function of Na+/mannose cotransport in rat kidney slices was low. [ABSTRACT FROM AUTHOR]

Published

2014

2. Regional distribution of SGLT activity in rat brain in vivo.

Author

Yu, Amy S., Hirayama, Bruce A., Timbol, Gerald, Jie Liu, Diez-Sampedro, Ana, Kepe, Vladimir, Satyamurthy, Nagichettiar, Sung-Cheng Huang, Wright, Ernest M., and Barrio, Jorge R.

Abstract

Na+-glucose cotransporter (SGLT) mRNAs have been detected in many organs of the body, but, apart from kidney and intestine, transporter expression, localization, and functional activity, as well as physiological significance, remain elusive. Using a SGLT-specific molecular imaging probe, α-methyl-4-deoxy-4-[18F]fluoro-D-glucopyranoside (Me-4-FDG) with ex vivo autoradiography and immunohistochemistry, we mapped in vivo the regional distribution of functional SGLTs in rat brain. Since Me-4-FDG is not a substrate for GLUT1 at the blood-brain barrier (BBB), in vivo delivery of the probe into the brain was achieved after opening of the BBB by an established procedure, osmotic shock. Ex vivo autoradiography showed that Me-4-FDG accumulated in regions of the cerebellum, hippocampus, frontal cortex, caudate nucleus, putamen, amygdala, parietal cortex, and paraventricular nucleus of the hypothalamus. Little or no Me-4-FDG accumulated in the brain stem. The regional accumulation of Me-4-FDG overlapped the distribution of SGLT1 protein detected by immunohistochemistry. In summary, after the BBB is opened, the specific substrate for SGLTs, Me-4-FDG, enters the brain and accumulates in selected regions shown to express SGLT1 protein. This localization and the sensitivity of these neurons to anoxia prompt the speculation that SGLTs may play an essential role in glucose utilization under stress such as ischemia. The expression of SGLTs in the brain raises questions about the potential effects of SGLT inhibitors under development for the treatment of diabetes. [ABSTRACT FROM AUTHOR]

Published

2013

3. Bridging the gap between structure and kinetics of human SGLT1.

Author

Sala-Rabanal, Monica, Hirayama, Bruce A., Loo, Donald D. F., Chaptal, Vincent, Abramson, Jeff, and Wright, Ernest M.

Abstract

The Na+-glucose cotransporter hSGLT1 is a member of a class of membrane proteins that harness Na+ electrochemical gradients to drive uphill solute transport. Although hSGLT1 belongs to one gene family (SLC5), recent structural studies of bacterial Na+ cotransporters have shown that Na+ transporters in different gene families have the same structural fold. We have constructed homology models of hSGLT1 in two conformations, the inward-facing occluded (based on vSGLT) and the outward open conformations (based on Mhp1), mutated in turn each of the conserved gates and ligand binding residues, expressed the SGLT1 mutants in Xenopus oocytes, and determined the functional consequences using biophysical and biochemical assays. The results establish that mutating the ligand binding residues produces profound changes in the ligand affinity (the halfsaturation concentration, K0.5); e.g., mutating sugar binding residues increases the glucose K0.5 by up to three orders of magnitude. Mutation of the external gate residues increases the Na+ to sugar transport stoichiometry, demonstrating that these residues are critical for efficient cotransport. The changes in phlorizin inhibition constant (Ki) are proportional to the changes in sugar K0.5, except in the case of F101C, where phlorizin Ki increases by orders of magnitude without a change in glucose K0.5. We conclude that glucose and phlorizin occupy the same binding site and that F101 is involved in binding to the phloretin group of the inhibitor. Substituted-cysteine accessibility methods show that the cysteine residues at the position of the gates and sugar binding site are largely accessible only to external hydrophilic methanethiosulfonate reagents in the presence of external Na+, demonstrating that the external sugar (and phlorizin) binding vestibule is opened by the presence of external Na+ and closes after the binding of sugar and phlorizin. Overall, the present results provide a bridge between kinetics and structural studies of cotransporters. [ABSTRACT FROM AUTHOR]

Published

2012

4. Structural selectivity of human SGLT inhibitors.

Author

Hummel, Charles S., Chuan Lu, Jie Liu, Ghezzi, Chiari, Hirayama, Bruce A., Loo, Donald D. F., Kepe, Vladimir, Barrio, Jorge R., and Wright, Ernest M.

Abstract

Human Na+-D-glucose cotransporter (hSGLT) inhibitors constitute the newest class of diabetes drugs, blocking up to 50% of renal glucose reabsorption in vivo. These drugs have potential for widespread use in the diabetes epidemic,but how they work at a molecular level is poorly understood. Here,we use electrophysiological methods to assess how they block Na+-D-glucose cotransporter SGLT1 and SGLT2 expressed in human embryonic kidney 293T (HEK-293T) cells and compared them to the classic SGLT inhibitor phlorizin. Dapagliflozin [(1S)-1,5,5-anhydro-1-C-{4-chloro-3-[(4-ethoxyphenyl) methyl]phenyl}-D-glucitol], two structural analogs, and the aglycones of phlorizin and dapagliflozin were investigated in detail. Dapagliflozin and fluoro-dapagliflozin [(1S)-1,5-anhydro-1-C-{4- chloro-3-[(4-ethoxyphenyl)methyl]phenyl}-4-F-4-deoxy-D-glucitol] blocked glucose transport and glucose-coupled currents with ≈100-fold specificity for hSGLT2 (Ki = 6 nM) over hSGLT1 (Ki = 400 nM). As galactose is a poor substrate for SGLT2, it was surprising that galacto-dapagliflozin [(1S)-1,5-anhydro-1-C-{4-chloro-3-[(4- ethoxyphenyl)methyl]phenyl}-D-galactitol] was a selective inhibitor of hSGLT2, but was less potent than dapagliflozin for both transporters (hSGLT2 Ki =25 nM, hSGLT1 Ki = 25,000 nM). Phlorizin and galacto-dapagliflozin rapidly dissociated from SGLT2 [half-time off rate (t1/2,Off) ≈ 20-30 s], while dapagliflozin and fluoro-dapagliflozin dissociated from hSGLT2 at a rate 10-fold slower (t1/2,Off ⩾ 180 s). Phlorizin was unable to exchange with dapagliflozin bound to hSGLT2. In contrast, dapagliflozin, fluoro-dapagliflozin, and galactodapagliflozin dissociated quickly from hSGLT1 (t1/2,Off = 1-2 s), and phlorizin readily exchanged with dapagliflozin bound to hSGLT1. The aglycones of phlorizin and dapagliflozin were poor inhibitors of both hSGLT2 and hSGLT1 with Ki values > 100 μM. These results show that inhibitor binding to SGLTs is composed of two synergistic forces: sugar binding to the glucose site, which is not rigid, and so different sugars will change the orientation of the aglycone in the access vestibule; and the binding of the aglycone affects the binding affinity of the entire inhibitor. Therefore, the pharmacophore must include variations in both the structure of the sugar and the aglycone. [ABSTRACT FROM AUTHOR]

Published

2012

5. Glucose transport by human renal Na+/D-glucose cotransporters SGLT1 and SGLT2.

Author

Hummel, Charles S., Lu, Chuan, Loo, Donald D. F., Hirayama, Bruce A., Voss, Andrew A., and Wright, Ernest M.

Subjects

CELL physiology, RENAL tubular transport, KIDNEY tubules, TYPE 2 diabetes treatment, TARGETED drug delivery, ELECTROPHYSIOLOGY, GLUCOSE

Abstract

The human Na+/D-glucose cotransporter 2 (hSGLT2) is believed to be responsible for the bulk of glucose reabsorption in the kidney proximal convoluted tubule. Since blocking reabsorption increases urinary glucose excretion, hSGLT2 has become a novel drug target for Type 2 diabetes treatment. Glucose transport by hSGLT2 was studied at 37°C in human embryonic kidney 293T cells using whole cell patch- clamp electrophysiology. We compared hSGLT2 with hSGLTI, the transporter in the straight proximal tubule (S3 segment). hSGLT2 transports with surprisingly similar glucose affinity and lower concentrative power than hSGLT1: Na+/D-glucose cotransport by hSGLT2 was electrogenic with apparent glucose and Na+ affinities of 5 and 25 mM, and a Na+:glucose coupling ratio of 1; hSGLT1 affinities were 2 and 70 mM and coupling ratio of 2. Both proteins showed voltage-dependent steady-state transport; however, unlike hSGLT1, hSGLT2 did not exhibit detectable pre-steady-state currents in response to rapid jumps in membrane voltage. D-Galactose was transported by both proteins, but with very low affinity by hSGLT2 (≥ 100 vs. 6 mM). β-D-Glucopyranosides were either substrates or blockers. Phlorizin exhibited higher affinity with hSGLT2 (Ki 11 vs. 140 nM) and a lower Off-rate (0.03 vs. 0.2 s-1) compared with hSGLT 1. These studies indicate that, in the early proximal tubule, hSGLT2 works at 50% capacity and becomes saturated only when glucose is ≥ 35 mM. Furthermore, results on hSGLT1 suggest it may play a significant role in the reabsorption of filtered glucose in the late proximal tubule. Our electrophysiological study provides groundwork for a molecular understanding of how hSGLT inhibitors affect renal glucose reabsorption. [ABSTRACT FROM AUTHOR]

Published

2011

6. Functional expression of SGLTs in rat brain.

Author

Yu, Amy S., Hirayama, Bruce A., Timbol, Gerald, Jie Liu, Basarah, Ernest, Kepe, Vladimir, Satyamurthy, Nagichettiar, Sung-Cheng Huang, Wright, Ernest M., and Barrio, Jorge R.

Subjects

*BRAIN, *GLUCOSE, *POSITRON emission tomography, *AUTORADIOGRAPHY, *HIPPOCAMPUS (Brain)

Abstract

This work provides evidence of previously unrecognized uptake of glucose via sodium-coupled glu- cose transporters (SGLT5) in specific regions of the brain. The current understanding of functional glucose utilization in brain is largely based on studies using positron emission tomography (PET) with the glucose tracer 2-deoxy-2-[F-l8]fluoro-D-glucose (2-FDG). However, 2-FDG is only a good substrate for facilitated-glucose transporters (GLUTs), not for SGLTs. Thus, glucose accumulation measured by 2-FDG omits the role of SGLTs. We designed and synthesized two high-affinity tracers: one, α-methyl-4-[F- 18]fluoro-4-deoxy-D-gluco- pyranoside (Me-4FDG), is a highly specific SGLT substrate and not transported by GLUTs; the other one, 4-[F-l8]fluoro-4-deoxy-o- glucose (4-FDa), is transported by both SGLTs and GLUTs and will pass through the blood brain barrier (BBB). In vitro Me-4FDG autoradiography was used to map the distribution of uptake by functional SGLTs in brain slices with a comparable result from in vitro 4-FDG autoradiography. Immunohistochemical assays showed that uptake was consistent with the distribution of SGLT protein. Ex vivo 4-FDa autoradiography showed that SGLTs in these areas are functionally active in the normal in vivo brain. The results establish that SGLTs are a normal part of the physiology of specific areas of the brain, including hippocampus, amygdala, hypothalamus, and cerebral cortices. 4-FDG PET imaging also established that this BBB-perme- able SGLT tracer now offers a functional imaging approach in humans to assess regulation of SGLT activity in health and disease. [ABSTRACT FROM AUTHOR]

Published

2010

7. Intestinal and renal Na+/glucose cotransporters share common structures.

Author

HIRAYAMA, BRUCE A., WONG, HELEN C., SMITH, CHARI D., HAGENBUCH, BRUNO A., HEDIGER, MATTHIAS A., and WRIGHT, ERNEST M.

Published

1991