Roles of Insulin Receptor Substrates (IRS) in renal function and renal hemodynamics

We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with rena...

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Published in	PLOS ONE Vol. 15; no. 12; p. e0242332
Main Authors	Hashimoto, Seiji, Maoka, Tomochika, Kawata, Tetsuya, Mochizuki, Toshio, Koike, Takao, Shigematsu, Takashi
Format	Journal Article
Language	English
Published	United States Public Library of Science (PLoS) 03.12.2020 Public Library of Science
Subjects	Abnormalities Albuminuria Albuminuria - blood Albuminuria - genetics Analysis Animals Aorta Biology and Life Sciences Blood Blood flow Blood Glucose Blood Glucose - genetics Creatinine Creatinine - blood Diabetes Diabetes mellitus Diabetes Mellitus, Type 2 Diabetes Mellitus, Type 2 - blood Diabetes Mellitus, Type 2 - genetics Diabetes Mellitus, Type 2 - pathology Diabetic Nephropathies Diabetic Nephropathies - blood Diabetic Nephropathies - genetics Diabetic Nephropathies - pathology Diabetic nephropathy Dosage and administration Engineering and Technology Experiments Genetic engineering Hemodynamic Monitoring Hemodynamic Monitoring - methods Hemodynamics Hospitals Hyperinsulinemia Hyperinsulinism Hyperinsulinism - blood Hyperinsulinism - genetics Hyperinsulinism - pathology Insulin Insulin - blood Insulin receptor substrate 1 Insulin Receptor Substrate Proteins Insulin Receptor Substrate Proteins - genetics Insulin receptors Insulin Resistance Insulin Resistance - genetics Internal medicine Kidney Kidney - blood supply Kidney - metabolism Kidney - pathology Kidney function tests Laboratory animals Losartan Male Measurement Medicine Medicine and Health Sciences Metabolic disorders Metabolic syndrome Metabolism Methods Mice Mice, Knockout Nephrology Nephropathy Perfusion Pioglitazone Prediabetic State Prediabetic State - blood Prediabetic State - genetics Prediabetic State - pathology Q R Rats Receptors Renal Circulation Renal Circulation - genetics Renal function Research Article Science Signal Transduction Signal Transduction - genetics Structure Substrates University graduates Urine Veins & arteries Japan United States > US
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ISSN	1932-6203 1932-6203
DOI	10.1371/journal.pone.0242332

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Abstract	We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout ( IRS1–/– ), and IRS2-knockout ( IRS2–/– ) mice. IRS2–/–mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1–/– and IRS2–/– groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (P sf ) were reduced in both the IRS1 -/- and IRS2 -/- . The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes.
AbstractList	We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout (IRS1-/-), and IRS2-knockout (IRS2-/-) mice. IRS2-/-mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1-/-and IRS2-/-groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (Psf) were reduced in both the IRS1 -/- and IRS2 -/-. The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes. We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout (IRS1-/-), and IRS2-knockout (IRS2-/-) mice. IRS2-/-mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1-/-and IRS2-/-groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (P.sub.sf) were reduced in both the IRS1 -/- and IRS2 -/-. The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes. We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout (IRS1-/-), and IRS2-knockout (IRS2-/-) mice. IRS2-/-mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1-/-and IRS2-/-groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (Psf) were reduced in both the IRS1 -/- and IRS2 -/-. The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes.We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout (IRS1-/-), and IRS2-knockout (IRS2-/-) mice. IRS2-/-mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1-/-and IRS2-/-groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (Psf) were reduced in both the IRS1 -/- and IRS2 -/-. The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes. We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats have hyperinsulinemia, insulin resistance and metabolic syndrome. It is well known that insulin resistance is frequently associated with renal abnormalities, but the mechanism underlying this association has remained speculative. Although insulin is known to modify renal hemodynamics, little is known about the roles of insulin receptor substrates (IRS1, IRS2) in the renal actions of insulin. To address this issue, the effects of insulin on renal function and renal hemodynamics were investigated in C57BL/6 (WT: wild type), insulin receptor substrate 1- knockout ( IRS1–/– ), and IRS2-knockout ( IRS2–/– ) mice. IRS2–/–mice had elevated glucose level as expected. 24-h urine collections and serum creatinine revealed that creatinine clearance did not significantly differ between these groups. Albuminuria was found in IRS1–/– and IRS2–/– groups. We examined the effects on the IRS during the administration of Losartan, which is widely used for diabetic nephropathy. After the administration of Losartan the IRS displayed improved renal hemodynamics. Moreover, the subjects were also given Pioglitazone, which improves insulin resistance. Losartan significantly reduced albuminuria in both groups. Pioglitazone also showed similar results. We assessed the autoregulatory responses of the total renal blood flow (RBF), the superficial (SBF) and the deep renal cortical blood flow (DBF) with stepwise reductions of renal perfusion pressure (RPP), which was induced by a manual clamp on the abdominal aorta. During the clamp induced reductions of the RPP by 10 to 20mm HG, RBF, SBF and the DBF fell significantly more in the IRS1 and IRS2 than in the WT mice. Furthermore micropuncture studies showded that compared to the WT tubuloglomerular feedback (TGF) responses of the stop flow pressure (P sf ) were reduced in both the IRS1 -/- and IRS2 -/- . The results of the IRS1 and IRS2 mice displayed the pressence of hemodynamic abnormalities. Losartan and Pioglitazone have shown the potential to improve these abnormalities. In conclusion the results indicate that IRS plays a major role in the stimulation of renal functions and renal hemodynamics in type type II diabetes.
Audience	Academic
Author	Takashi Shigematsu Seiji Hashimoto Toshio Mochizuki Tomochika Maoka Takao Koike Tetsuya Kawata
AuthorAffiliation	1 Department of Nephrology, Kinan Hospital, Tanabe, Wakayama Prefecture, Japan 4 Department of Nephrology, Wakayama Medical University, Wakayama, Wakayama Prefecture, Japan University Medical Center Utrecht, NETHERLANDS 2 NTT East Japan Sapporo Hospital Department of Nephrology, Chuou-ku, Sapporo, Japan 3 Hokkaido University Graduate School of Medicine, Internal Medicine II, Kita-ku, Sapporo, Japan
AuthorAffiliation_xml	– name: University Medical Center Utrecht, NETHERLANDS – name: 2 NTT East Japan Sapporo Hospital Department of Nephrology, Chuou-ku, Sapporo, Japan – name: 3 Hokkaido University Graduate School of Medicine, Internal Medicine II, Kita-ku, Sapporo, Japan – name: 4 Department of Nephrology, Wakayama Medical University, Wakayama, Wakayama Prefecture, Japan – name: 1 Department of Nephrology, Kinan Hospital, Tanabe, Wakayama Prefecture, Japan
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Notes	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23 Current address: Fourth Department of Internal Medicine, Tokyo Women's Medical University, Tokyo, Japan Competing Interests: The authors have declared that no competing interests exist.
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Snippet	We have reported previously that renal hemodynamic abnormalities exist in the prediabetic stage of type II diabetic rats. At this prediabetic stage these rats...
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SubjectTerms	Abnormalities Albuminuria Albuminuria - blood Albuminuria - genetics Analysis Animals Aorta Biology and Life Sciences Blood Blood flow Blood Glucose Blood Glucose - genetics Creatinine Creatinine - blood Diabetes Diabetes mellitus Diabetes Mellitus, Type 2 Diabetes Mellitus, Type 2 - blood Diabetes Mellitus, Type 2 - genetics Diabetes Mellitus, Type 2 - pathology Diabetic Nephropathies Diabetic Nephropathies - blood Diabetic Nephropathies - genetics Diabetic Nephropathies - pathology Diabetic nephropathy Dosage and administration Engineering and Technology Experiments Genetic engineering Hemodynamic Monitoring Hemodynamic Monitoring - methods Hemodynamics Hospitals Hyperinsulinemia Hyperinsulinism Hyperinsulinism - blood Hyperinsulinism - genetics Hyperinsulinism - pathology Insulin Insulin - blood Insulin receptor substrate 1 Insulin Receptor Substrate Proteins Insulin Receptor Substrate Proteins - genetics Insulin receptors Insulin Resistance Insulin Resistance - genetics Internal medicine Kidney Kidney - blood supply Kidney - metabolism Kidney - pathology Kidney function tests Laboratory animals Losartan Male Measurement Medicine Medicine and Health Sciences Metabolic disorders Metabolic syndrome Metabolism Methods Mice Mice, Knockout Nephrology Nephropathy Perfusion Pioglitazone Prediabetic State Prediabetic State - blood Prediabetic State - genetics Prediabetic State - pathology Q R Rats Receptors Renal Circulation Renal Circulation - genetics Renal function Research Article Science Signal Transduction Signal Transduction - genetics Structure Substrates University graduates Urine Veins & arteries
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Title	Roles of Insulin Receptor Substrates (IRS) in renal function and renal hemodynamics
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