The effects of KATP channel modulators on counterregulatory responses and cognitive function during acute controlled hypoglycaemia in healthy men: a pilot study.

AIMS: To examine the effects of agents that alter potassium adenosine triphosphate (KATP) channel activity in beta-cells on cognitive function and counterregulatory hormone responses during acute hypoglycaemia, given the physiological similarities between the pancreatic beta-cell and the hypothalamic glucose-sensitive neurones (GSN) and the widespread distribution of sulphonylurea receptors in neuronal cells throughout the brain. METHODS: Ten healthy males were studied on four occasions and in random order underwent three stepped hypoglycaemic (plasma glucose aims: 3.4, 2.8, 2.4 mmol/l) and one euglycaemic (plasma glucose aim: 5 mmol/l) insulin clamps. Prior to each hypoglycaemic study, volunteers received either 10 mg glibenclamide, or 5 mg/kg diazoxide or placebo orally. Cognitive function, symptom scores and counterregulatory hormone responses were measured at each glycaemic level. RESULTS: There was no statistically significant effect of either drug on the symptoms generated or the counterregulatory hormonal response during hypoglycaemia. However, cognitive function was better preserved during hypoglycaemia in the glibenclamide-treated arm, particularly four-choice reaction time which deteriorated at a plasma glucose 2.5 mmol/l compared with 3.0 mmol/l with diazoxide (P = 0.015) and 2.9 mmol/l with placebo (P = 0.114). CONCLUSIONS: Single doses of pharmacological agents which alter membrane KATP channel activity do not affect the counterregulatory response to hypoglycaemia but may modify cognitive function during cerebral glucopenia. The unexpected effects of glibenclamide on cortical function suggest a novel action of sulphonylureas that warrants further investigation.     

心肌线粒体ATP敏感性钾通道开放保护线粒体结构和功能

目的　评价线粒体ATP敏感性钾通道 (mitoKATP)开放剂二氮嗪对缺氧心肌线粒体结构和功能的影响。方法　异丙肾上腺素 (ISO)皮下注射诱发大鼠心肌缺氧损伤 ,观察二氮嗪对线粒体呼吸控制比 (RCR)、膜流动性、磷脂酶A2 和磷脂含量的影响。结果　ISO皮下注射诱发大鼠心肌缺氧损伤后 ,与对照组比较线粒体RCR降低了 2 0 8% (P <0 0 1) ,膜流动性降低了 9 1% (P <0 0 5 ) ,磷脂酶A2 活性增加了14 4 5 % (P <0 0 1) ,磷脂含量下降了 37 5 % (P <0 0 5 ) ,二氮嗪预防性给药后可改善RCR、膜流动性和磷脂含量。结论　二氮嗪可保护心肌缺氧损伤后线粒体膜结构和功能的完整     

A Combination of Nifedipine and OctreotideTreatment in an HyperinsulinemicHypoglycemic Infant

Hyperinsulinemic hypoglycemia (HH) is the commonest cause of persistent hypoglycemia in the neonatal and infancy periods. Mutations in the ABCC8 and KCNJ11 genes, which encode subunits of the ATP-sensitive potassium channel in the pancreatic beta cell, are identified in approximately 50% of these patients. The first-line drug in the treatment of HH is diazoxide. Octreotide and glucagon can be used in patients who show no response to diazoxide. Nifedipine, a calcium-channel blocker, has been shown to be an effective treatment in a small number of patients with diazoxide-unresponsive HH. We report a HH patient with a homozygous ABCC8 mutation (p.W1339X) who underwent a near-total pancreatectomy at 2 months of age due to a lack of response to diazoxide and octreotide treatment. Severe hypoglycemic attacks continued following surgery, while the patient was being treated with octreotide. These attacks resolved when nifedipine was introduced. Whilst our patient responded well to nifedipine, the dosage could not be increased to 0.75 mg/kg/day due to development of hypotension, a reported side effect of this drug. Currently, our patient, now aged 4 years, is receiving a combination of nifedipine and octreotide treatment. He is under good control and shows no side effects. In conclusion, nifedipine treatment can be started in patients with HH who show a poor response to diazoxide and octreotide treatment.     

Opening of ATP-sensitive potassium channels causes generation of free radicals in vascular smooth muscle cells

Recent evidence suggests that opening of mitochondrial K_ATP channels in cardiac muscle triggers the preconditioning phenomenon through free radical production. The present study tested the effects of K_ATP channel openers in a vascular smooth muscle cell model using the fluorescent probe MitoTracker (MTR) Red™ for detection of reactive oxygen species (ROS). Rat aortic smooth muscle cells (A7r5) were incubated with 1 μM reduced MTR (non-fluorescent) and the MTR oxidation product (fluorescent) was quantified. Thirty-minute pretreatment with either diazoxide (200 μM) or pinacidil (100 μM), both potent mitochondrial K_ATP channel openers, increased fluorescent intensity (FI) to 149 and 162 % of control (p < 0.05 for both), respectively, and the K_ATP channel inhibitor 5-hydroxydecanoate (5HD) blocked it. Valinomycin, a potassium-selective ionophore, raised FI to 156 % of control (p <: 0.05). However, 5HD did not affect the valinomycin-induced increase in FI. Inhibition of mitochondrial electron transport (myxothiazol) or uncoupling of oxidative phosphorylation (dinitrophenol) also blocked either valinomycin- or diazoxide-induced increase in FI, and free radical scavengers prevented any diazoxide-mediated increase in fluorescence. Finally the diazoxide-induced increase in fluorescence was not blocked by the PKC inhibitor chelerythrine, but was by HMR 1883, a putative surface K_ATP channel blocker. Thus opening of K_ATP channels increases generation of ROS via the mitochondrial electron transport chain in vascular smooth muscle cells. Furthermore, a potassium-selective ionophore can mimic the effect of putative mitochondrial KATP channel openers. We conclude that potassium movement through KATP directly leads to ROS production by the mitochondria. Received: 7 January 2002, Returned for revision: 31 January 2002, Revision received: 21 February 2002, Accepted: 14 March 2002     

Age-related impairment of cerebral blood flow response to KATP channel opener in Alzheimer’s disease mice with presenilin-1 mutation

Local cerebral blood flow (CBF) responses to neuronal activity are essential for cognition and impaired CBF responses occur in Alzheimer’s disease (AD). In this study, regional CBF (rCBF) responses to the K_ATP channel opener diazoxide were investigated in 3xTgAD, WT and mutant Presenilin 1(PS1_M146V) mice from three age groups using Laser-Doppler flowmetry. The rCBF response was reduced early in young 3xTgAD mice and almost absent in old 3xTgAD mice, up to 30%–40% reduction with altered CBF velocity and mean arterial pressure versus WT mice. The impaired rCBF response in 3xTgAD mice was associated with progression of AD pathology, characterized by deposition of intracellular and vascular amyloid-β (Aβ) oligomers, senile plaques and tau pathology. The nitric oxide synthase (NOS) inhibitor N^ω-nitro-L-arginine abolished rCBF response to diazoxide suggesting NO was involved in the mediation of vasorelaxation. Levels of phosphor-eNOS (Ser1177) diminished in 3xTgAD brains with age, while the rCBF response to the NO donor sodium nitroprusside remained. In PS1_M146V mice, the rCBF response to dizoxide reduced and high molecular weight Abeta oligomers were increased indicating PS1_M146V contributed to the dysregulation of rCBF response in AD mice. Our study revealed an Aβ oligomer-associated compromise of cerebrovascular function in rCBF response to diazoxide in AD mice with PS1_M146V mutation.     

Studies on the mechanism of xylitol-induced insulin secretion in dogs

Summary The effect of infusion of small doses of xylitol into the pancreatic artery upon insulin release was studied in anaesthetized dogs, in order to decide whether the strong insulin-releasing effect of xylitol in dogs is mediated by a direct action of xylitol upon the islets or indirectly by some of its metabolites. Xylitol or glucose was infused at 0.5–1.0 mg/kg · min either into the femoral vein or into the superior pancreaticoduodenal artery, and the changes in plasma insulin were measured in the superior pancreaticoduodenal vein. Infusion into the pancreatic artery always resulted in a sharp increase in insulin release, whereas intravenous infusion caused no or little increase. Infusion of xylitol into the superior pancreaticoduodenal artery produced a prompt increase in plasma insulin in the superior pancreaticoduodenal vein but not in the splenic vein. These data suggest that xylitol has a direct stimulatory effect upon islet cells. — During intravenous infusion of epinephrine (1.0 g/kg. min), plasma insulin did not increase despite intravenous administration of glucose or xylitol (0.4 g/kg). There was a rebound rise of plasma insulin after cessation of epinephrine infusion. Plasma insulin responses to intravenous injection of glucose or xylitol (0.4 g/kg) were inhibited also by the intravenous infusion of diazoxide (0.2 mg/kg · min), but this was somewhat variable among individual dogs. The suppression by epinephrine or diazoxide of both glucose and xylitol-induced hyperinsulinaemia may suggest that there is some common mechanism between the insulin-releasing effects of glucose and xylitol.

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Untersuchungen zum Mechanismus der verstärkten Insulinsekretion unter Xylit

Zusammenfassung An anaesthesierten Hunden wurde die Wirkung der Infusion kleiner Xylit-Mengen in die Pankreasarterie auf die Insulinfreisetzung untersucht, um zu klären, ob das Xylit direkt oder über einen seiner Metabolite auf die Insulinausschüttung wirkt. Xylit oder Glucose wurde in Mengen von 0.5–1.0 mg/kg/min entweder in die Femoralvene oder in die A.pankreaticoduodenalis sup. infundiert und die Änderung des PlasmaInsulins in der V.pankreatico-duodenalis sup. gemessen. Zufuhr über die Pankreasarterie löste immer eine abrupte Steigerung der Insulinfreisetzung aus, während intravenöse Gaben zu keinem oder nur einem geringen Anstieg führten. Die Xylit-Infusion in die A.pankreaticoduodenalis sup.bewirkte zwar eine prompte Steigerung der Plasma-Insulinspiegel in der V.pankreatico duodenalis sup., nicht aber in der Milzvene. — Diese Befunde sprechen dafür, daß Xylit die Inselzellen direkt stimuliert. Während einer i.v.Infusion von 1.0 g/kg/min Adrenalin stieg das Plasma-Insulin trotz intravenöser Zufuhr von 0.4 g/kg Glucose oder Xylit nicht an. Nach Beendigung der Adrenalin-Infusion wurde ein verstärkter Wiederanstieg des Plasma-Insulins beobachtet. Auch durch i.v.Gaben von 0.2 mg/kg/min Diazoxid ließ sich die Wirkung der Infusion von 0.4 g/kg Glucose oder Xylit unterdrükken, wobei sich jedoch Unterschiede zwischen den einzelnen Tieren ergaben. Die Aufhebung des Xylit- u. Glucose-Effektes auf die Insulinsekretion durch Adrenalin und Diazoxid könnte darauf hinweisen, daß die Steigerung der Insulinfreisetzung durch Glucose und Xylit auf einem gemeinsamen Mechanismus beruht.

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Etudes sur le mécanisme de la sécrétion d'insuline provoquée par le xylitol chez des chiens

Résumé L'effet sur la sécrétion d'insuline de l'infusion de petites doses de xylitol dans l'artère pancréatique a été étudié chez des chiens anesthésiés, afin de savoir si l'effet fortement insulino-sécréteur du xylitol chez les chiens est dû à une action directe du xylitol sur les îlots ou à une action indirecte par l'intermédiaire de certains de ses métabolites. Le xylitol ou le glucose était infusé la dose de 0.5–1.0 mg/kg. min, soit dans la veine fémorale, soit dans l'artère pancréatico-duodénale supérieure, et les variations de l'insuline plasmatique étaient mesurées dans la veine pancréatico-duodénale supérieure. L'infusion dans l'artère pancréatique provoquait toujours une rapide augmentation de la sécrétion d'insuline, tandis que l'infusion intraveineuse ne causait pas ou peu d'augmentation. L'infusion de xylitol dans l'artère pancréaticoduodénale supérieure provoquait une augmentation prompte de l'insuline plasmatique dans la veine pancréatico-duodénale supérieure, mais pas dans la veine splénique. Ces données suggèrent que le xylitol a un effet stimulateur direct sur les cellules des îlots. — Pendant l'infusion intraveineuse d'adrénaline (1.0 g/kg. min), l'insuline plasmatique n'augmentait pas malgré l'administration intraveineuse de glucose ou de xylitol (0.4 g/kg). Après l'arrêt de l'infusion d'adrénaline, l'insuline plasmatique présentait un phénomène de rebound. Les réponses de l'insuline plasmatique l'injection intraveineuse de glucose ou de xylitol (0.4 g/kg) étaient également inhibées par l'infusion intraveineuse de diazoxide (0.2 mg/ kg. min), mais ceci était un peu variable selon les chiens. La suppression par l'adrénaline ou le diazoxide de l'hyperinsulinémie provoquée par le glucose et le xylitol peut suggérer qu'il existe un mécanisme commun entre les effets insulino-sécréteurs du glucose et du xylitol.

     

Cardioprotective effects of mitochondrial KATP channels activated at different time

Backgroud Recent studies in adult hearts have indicated that KATP channels in the inner mitochondrial membrance are responsible for the protection. And we investigated whether opening of mitochondrial KATP channels (mKATP) could provide myocardial protection for immature rabbits and determined its role in cardioprotection.Methods Thirty-four 3-4-week-old rabbits, weighing 300-350 g, were divided randomly into five groups: Group Ⅰ (control group, n=8); Group Ⅱ ［diazoxide preconditioning group; n=8; the hearts were pretreated with 100 μmol/L diazoxide for 5 minutes followed by 10-minute wash out with Krebs-Henseleit buffer (KHB)］; Group Ⅲ ［diazoxide+5-hydroxydeconate (5-HD) preconditioning group; n=5; the hearts were pretreated with 100 μmol/L diazoxide and 100 μmol/L 5-HD); Group Ⅳ (diazoxide+cardioplegia group; n=8; cardioplegia containing 100 μmol/L diazoxide perfused the hearts for 5 minutes before ischemia); Group Ⅴ (diazoxide+5-HD+cardioplegia group; n=5; the cardioplegia contained 100 μmol/L diazoxide and 100 μmol/L 5-HD). All hearts were excised and connected to langendrff perfusion system and passively perfused with KHB at 38℃ under a pressure of 70 cmH2O. After reperfusion, the recovery rate of left ventricular diastolic pressure (LVDP), ±dp/dtmax, coronary flow (CF), the creatinine kinase (CK), lactate dehydrogenase (LDH), aspartate aminotransferase (AST) in coronary sinus venous effluent and the tissue ATP were measured. Mitochondria were evaluated semiquantitatively by morphology.Results After ischemia and reperfusion (I/R), the two groups that were treated by diazoxide only (Groups Ⅱ and Ⅳ) had a significant improvement in LVDP, ±dp/dtmax, and CF recovery. AST, LDH, and CK were decreased, and the levels of tissue ATP in the two groups were higher. Mitochondria was protected better in Group Ⅳ than in other groups. Conclusions Activating mKATP channels before and during ischemia can similarly protect immature rabbit hearts, and the mechanism is related to the direct protective effect on mitochondria. Opening of mKATP channel during ischemia provides a better protection for mitochondria than it does before ischemia.     

二氮嗪后处理对缺氧复氧成年大鼠心肌细胞保护作用的体外研究

目的研究线粒体ATP-敏感性钾通道（mitoKTP）开放剂二氮嗪（diazoxide,DZ）后处理对缺氧复氧成年大鼠心肌细胞的影响。方法体外培养原代成年大鼠心肌细胞建立缺氧复氧损伤模型,随机分为5组：Normal组（在CO2培养箱中持续培养6h）;H／R组（缺氧3h复氧3h）;DZ组（缺氧3h复氧3h,在复氧5min时给予100mol／LDZ）;DZ＋5-羟葵酸盐（5-hydmxydecanoate,5-HD）组（缺氧3h复氧3h,在缺氧末给予100mol／L选择性mitoK。通道阻断剂5-HD,然后在复氧5min时给予100mol／LDZ）;5-HD组（缺氧3h复氧3h,在缺氧末给予100mol／L5-HD）。复氧3h末检测各组培养基中乳酸脱氢酶（LDH）漏出量和丙二醛（MDA）含量,TUNEL法测定心肌细胞凋亡指数、测定心肌细胞收缩幅度。结果与Normal组相比,其他4组培养基中LDH漏出量和MDA含量明显升高,心肌细胞凋亡指数也显著增高,心肌细胞收缩幅度降低（P〈0．05）;与H／R组比较,DZ后处理使培养基中LDH漏出量及MDA含量减少、心肌细胞凋亡指数降低,复氧后心肌细胞收缩幅度明显增高（P〈0．05）,但是缺氧末即刻给予5-HD可以逆转DZ的作用（P〈0．05）;5-HD组与H／R组相比各指标差异无统计学意义（P〉0．05）。结论Dz后处理可以通过开放mitoK。通道对缺氧复氧成年大鼠心肌细胞发挥保护作用。     

二氮嗪预处理对肝硬化大鼠肝脏的保护作用

目的探讨采用线粒体ATP敏感性钾通道(mitoKATP通道)选择性开放剂二氮嗪(DE)进行预处理能否模拟缺血预处理(IP)对硬化肝脏缺血再灌注损伤的保护作用及其可能的作用机制。方法雄性肝硬化SD大鼠随机分为5组(每组8只)。IP组以肝缺血5 min作预处理;DE组以静脉注射DE作为预处理;DE 5-HD组是在DE组基础上再予静注mitoKATP通道选择性阻滞剂5-hydroxydecanoate(5-HD)进行预处理;对照组(C组)以静注等量生理盐水作为预处理;上述4组均在预处理后行肝缺血45 min再灌注60 min;缺血方式均为70%肝脏热缺血。假手术组(S组)仅行开腹,不作任何其他处理。完成预定实验操作后分别取血用于血清谷丙转氨酶(ALT)与乳酸脱氢酶(LDH)检测,切取肝组织用于测定ATP酶活力、湿重/干重(W/D)的测定及观察显微、超微结构变化。结果C组ALT,LDH,ATP酶及W/D的水平明显高于S组(P<0.01),肝脏的显微及超微结构损伤明显;IP组与DE组的各项肝组织损伤指标均明显好于C组,ATP酶活性低于C组(P<0.05及P<0.01);而DE 5-HD组的肝损伤指标均差于DE组,ATP酶活性高于DE组(P<0.05及P<0.01)。结论使用DE进行药物预处理能够模拟出IP效应,对肝硬化大鼠肝脏I/R损伤具有保护作用,其作用可能与下调肝组织ATP酶活性,减少ATP大量分解,使肝组织ATP含量升高,改善肝能量代谢,增加能量储备;改善肝组织微循环,减轻肝脏水肿有关。