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Diabetologia

Erschienen in:

01.04.2006 | Article

Vascular and metabolic effects of methacholine in relation to insulin action in muscle

verfasst von: H. Mahajan, C. M. Kolka, J. M. B. Newman, S. Rattigan, S. M. Richards, M. G. Clark

Erschienen in: Diabetologia | Ausgabe 4/2006

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Abstract

Aims/hypothesis

Methacholine (MC) is a nitric oxide vasodilator, but unlike other vasodilators, it potentiates insulin-mediated glucose uptake by muscle. The present study aimed to resolve whether this action was the result of a vascular effect of MC leading to increased muscle perfusion or a direct effect of MC on the myocytes. We hypothesise that vascular-mediated insulin-stimulated glucose uptake responses to MC occur at lower doses than direct myocyte MC-mediated increases in glucose uptake.

Methods

The vascular and metabolic effects of this vasodilator were examined in rats in vivo using a novel local infusion technique, and in the pump-perfused rat hindlimb under conditions of constant flow.

Results

Local infusion of low-dose MC (0.3 μmol/l) into the epigastric artery of one leg (test) in vivo markedly increased femoral blood flow and decreased vascular resistance, without effects in the contra-lateral leg. Capillary recruitment, but not glucose uptake, was increased in the test leg. All increases caused by MC were confined to the test leg and blocked by local infusion into the test leg of N-nitro-l-arginine methyl ester (l-NAME), but not by infusion of N-nitro-d-arginine methyl ester (d-NAME). In the constant-flow pump-perfused rat hindlimb, infusion of 0.6 μmol/l MC vasodilated the pre-constriction effected by 70 nmol/l noradrenaline or 300 nmol/l serotonin, and this was blocked by 10 μmol/l l-NAME. 2-Deoxyglucose in muscle was increased by 30 μmol/l MC (p<0.05), but was unaffected by 3 μmol/l MC. All increases in 2-deoxyglucose uptake by 30 μmol/l MC were blocked by 10 μmol/l l-NAME.

Conclusions/interpretation

MC has dose-dependent effects both on the vasculature and on muscle metabolism. At low dose (0.3–3 μmol/l), MC is a potent vasodilator in muscle, both in vivo and in vitro, without metabolic effects; at higher doses (≥30 μmol/l) MC has a direct metabolic effect leading to increased glucose uptake. Both the vascular and metabolic effects are sensitive to l-NAME. The low-dose enhancement of insulin action in vivo by MC, which has been reported previously, thus seems to be attributable to vascular effects.

Anderson TJ, Meredith IT, Ganz P, Selwyn AP, Yeung AC (1994) Nitric oxide and nitrovasodilators: similarities, differences and potential interactions. J Am Coll Cardiol 24:555–566PubMedCrossRef

Steinberg HO, Brechtel G, Johnson A, Fineberg N, Baron AD (1994) Insulin-mediated skeletal muscle vasodilation is nitric oxide dependent. A novel action of insulin to increase nitric oxide release. J Clin Invest 94:1172–1179PubMed

Sarabi M, Lind L, Millgard J et al (1999) Local vasodilatation with metacholine, but not with nitroprusside, increases forearm glucose uptake. Physiol Res 48:291–295PubMed

Etgen GJJ, Fryburg DA, Gibbs EM (1997) Nitric oxide stimulates skeletal muscle glucose transport through a calcium/contraction- and phosphatidylinositol-3-kinase-independent pathway. Diabetes 46:1915–1919PubMedCrossRef

Young ME, Radda GK, Leighton B (1997) Nitric oxide stimulates glucose transport and metabolism in rat skeletal muscle in vitro. Biochem J 322:223–228PubMed

Natali A, Bonadonna R, Santoro D et al (1994) Insulin resistance and vasodilation in essential hypertension. Studies with adenosine. J Clin Invest 94:1570–1576PubMedCrossRef

Nuutila P, Raitakari M, Laine H et al (1996) Role of blood flow in regulating insulin-stimulated glucose uptake in humans. Studies using bradykinin, [¹⁵O]water, and [¹⁸F]fluoro-deoxy-glucose and positron emission tomography. J Clin Invest 97:1741–1747PubMed

Natali A, Quinones GA, Pecori N, Sanna G, Toschi E, Ferrannini E (1998) Vasodilation with sodium nitroprusside does not improve insulin action in essential hypertension. Hypertension 31:632–636PubMed

Pendergrass M, Fazioni E, Collins D, Defronzo RA (1998) IGF-I increases forearm blood flow without increasing forearm glucose uptake. Am J Physiol 275:E345–E350PubMed

10.

Rattigan S, Clark MG, Barrett EJ (1997) Hemodynamic actions of insulin in rat skeletal muscle: evidence for capillary recruitment. Diabetes 46:1381–1388PubMedCrossRef

11.

Baron AD, Tarshoby M, Hook G et al (2000) Interaction between insulin sensitivity and muscle perfusion on glucose uptake in human skeletal muscle: evidence for capillary recruitment. Diabetes 49:768–774PubMedCrossRef

12.

Renkin EM (1984) Control of microcirculation and blood–tissue exchange. In: Renkin EM, Michel CC, Geiger SR (eds) Handbook of physiology—the cardiovascular system IV. American Physiological Society, Bethesda, 627–687

13.

Mahajan H, Richards SM, Rattigan S, Clark MG (2004) Local methacholine but not bradykinin potentiates insulin-mediated glucose uptake in muscle in vivo by augmenting capillary recruitment. Diabetologia 47:2226–2234CrossRefPubMed

14.

Kraegen EW, James DE, Jenkins AB, Chisholm DJ (1985) Dose-response curves for in vivo insulin sensitivity in individual tissues in rats. Am J Physiol 248:E353–E362PubMed

15.

James DE, Jenkins AB, Kraegen EW (1985) Heterogeneity of insulin action in individual muscles in vivo: euglycemic clamp studies in rats. Am J Physiol 248:E567–E574PubMed

16.

Ruderman NB, Houghton CR, Hems R (1971) Evaluation of the isolated perfused rat hindquarter for the study of muscle metabolism. Biochem J 124:639–651PubMed

17.

Colquhoun EQ, Hettiarachchi M, Ye JM et al (1988) Vasopressin and angiotensin II stimulate oxygen uptake in the perfused rat hindlimb. Life Sci 43:1747–1754CrossRefPubMed

18.

Clark MG, Colquhoun EQ, Rattigan S et al (1995) Vascular and endocrine control of muscle metabolism. Am J Physiol 268:E797–E812PubMed

19.

Zhang L, Vincent MA, Richards SM et al (2004) Insulin sensitivity of muscle capillary recruitment in vivo. Diabetes 53:447–453PubMedCrossRef

20.

Halseth AE, Bracy DP, Wasserman DH (2000) Limitations to basal and insulin-stimulated skeletal muscle glucose uptake in the high-fat-fed rat. Am J Physiol 279:E1064–E1071

21.

Holmang A, Muller M, Andersson OK, Lonnroth P (1998) Minimal influence of blood flow on interstitial glucose and lactate-normal and insulin-resistant muscle. Am J Physiol 274:E446–E452PubMed

22.

Grubb B, Snarr JF (1977) Effect of flow rate and glucose concentration on glucose uptake rate by the rat limb. Proc Soc Exp Biol Med 154:33–36PubMed

23.

Baron AD (1994) Hemodynamic actions of insulin. Am J Physiol 267:E187–E202PubMed

24.

Natali A (1997) Skeletal muscle blood flow and insulin action. Nutr Metab Cardiovasc Dis 7:105–109

25.

26.

Chavoshan B, Sander M, Sybert TE, Hansen J, Victor RG, Thomas GD (2002) Nitric oxide-dependent modulation of sympathetic neural control of oxygenation in exercising human skeletal muscle. J Physiol 540:377–386CrossRefPubMed

27.

Vincent MA, Barrett EJ, Lindner JR, Clark MG, Rattigan S (2003) Inhibiting NOS blocks microvascular recruitment and blunts glucose uptake in response to insulin. Am J Physiol 285:E123–E129

28.

Vincent MA, Clerk LH, Lindner JR et al (2004) Microvascular recruitment is an early insulin effect that regulates skeletal muscle glucose uptake in vivo. Diabetes 53:1418–1423PubMedCrossRef

29.

Baron AD, Steinberg HO, Chaker H, Leaming R, Johnson A, Brechtel G (1995) Insulin-mediated skeletal muscle vasodilation contributes to both insulin sensitivity and responsiveness in lean humans. J Clin Invest 96:786–792PubMed

30.

Scherrer U, Randin D, Vollenweider P, Vollenweider L, Nicod P (1994) Nitric oxide release accounts for insulin’s vascular effects in humans. J Clin Invest 94:2511–2515PubMed

31.

Shankar R, Zhu JS, Ladd B, Henry D, Shen HQ, Baron AD (1998) Central nervous system nitric oxide synthase activity regulates insulin secretion and insulin action. J Clin Invest 102:1403–1412PubMedCrossRef

32.

Vicent D, Ilany J, Kondo T et al (2003) The role of endothelial insulin signaling in the regulation of vascular tone and insulin resistance. J Clin Invest 111:1373–1380CrossRefPubMed

33.

Frandsen U, Bangsbo J, Sander M et al (2001) Exercise-induced hyperaemia and leg oxygen uptake are not altered during effective inhibition of nitric oxide synthase with N(G)-nitro-l-arginine methyl ester in humans. J Physiol 531:257–264CrossRefPubMed

34.

Bradley SJ, Kingwell BA, McConell GK (1999) Nitric oxide synthase inhibition reduces leg glucose uptake but not blood flow during dynamic exercise in humans. Diabetes 48:1815–1821PubMedCrossRef

35.

Bruning TA, Hendriks MG, Chang PC, Kuypers EA, van Zwieten PA (1994) In vivo characterization of vasodilating muscarinic-receptor subtypes in humans. Circ Res 74:912–919PubMed

36.

Bruning TA, Chang PC, Hendriks MG, Vermeij P, Pfaffendorf M, van Zwieten PA (1995) In vivo characterization of muscarinic receptor subtypes that mediate vasodilatation in patients with essential hypertension. Hypertension 26:70–77PubMed

37.

Hendriks MG, Pfaffendorf M, van Zwieten PA (1993) Characterization of the muscarinic receptors in the mesenteric vascular bed of spontaneously hypertensive rats. J Hypertens 11:1329–1335PubMedCrossRef

38.

McCulloch AI, Bottrill FE, Randall MD, Hiley CR (1997) Characterization and modulation of EDHF-mediated relaxations in the rat isolated superior mesenteric arterial bed. Br J Pharmacol 120:1431–1438PubMedCrossRef

39.

Matsui M, Motomura D, Karasawa H et al (2000) Multiple functional defects in peripheral autonomic organs in mice lacking muscarinic acetylcholine receptor gene for the M3 subtype. Proc Natl Acad Sci U S A 97:9579–9584CrossRefPubMed

40.

Matsui M, Motomura D, Fujikawa T et al (2002) Mice lacking M2 and M3 muscarinic acetylcholine receptors are devoid of cholinergic smooth muscle contractions but still viable. J Neurosci 22:10627–10632PubMed

Titel: Vascular and metabolic effects of methacholine in relation to insulin action in muscle
verfasst von: H. Mahajan
C. M. Kolka
J. M. B. Newman
S. Rattigan
S. M. Richards
M. G. Clark
Publikationsdatum: 01.04.2006
Verlag: Springer-Verlag
Erschienen in: Diabetologia / Ausgabe 4/2006
Print ISSN: 0012-186X
Elektronische ISSN: 1432-0428
DOI: https://doi.org/10.1007/s00125-005-0110-6

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