Clinical Efficacy of Fidarestat, a Novel Aldose Reductase Inhibitor, for Diabetic Peripheral Neuropathy

Hotta, Nigishi; Toyota, Takayoshi; Matsuoka, Kempei; Shigeta, Yukio; Kikkawa, Ryuichi; Kaneko, Toshio; Takahashi, Akira; Sugimura, Kimiya; Koike, Yasuo; Ishii, Jun; Sakamoto, Nobuo

doi:10.2337/diacare.24.10.1776

Cited by 205 publications

(121 citation statements)

References 27 publications

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“…The results, consistent with previous reports on the alleviation of diabetic complications with fidarestat treatment (63)(64)(65)(66), support a pathogenetic, rather than protective, role for increased aldose reductase activity in diabetic cataractogenesis and early retinopathy, and provide a rationale for the development of aldose reductase inhibitors, and, in particular, fidarestat, for their prevention and treatment.…”

Section: Discussionsupporting

confidence: 80%

Aldose reductase inhibitor fidarestat counteracts diabetes-associated cataract formation, retinal oxidative-nitrosative stress, glial activation, and apoptosis

Drel

Pacher²,

Ali³

et al. 2008

Int J Mol Med

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Abstract. This study was aimed at evaluating the potent and specific aldose reductase inhibitor fidarestat, on diabetesassociated cataract formation, and retinal oxidative-nitrosative stress, glial activation, and apoptosis. Control and streptozotocin-diabetic rats were treated with or without fidarestat (16 mg kg -1 d -1 ) for 10 weeks after an initial 2-week period without treatment. Lens changes were evaluated by indirect ophthalmoscopy and portable slit lamp. Nitrotyrosine, poly(ADP-ribose), and glial fibrillary acidic protein expression were assessed by immunohistochemistry. The rate of apoptosis was quantified in flat-mounted retinas by TUNEL assay with immunoperoxidase staining. To dissect the effects of high glucose exposure in retinal microvascular cells, primary bovine retinal pericytes and endothelial cells were cultured in 5 or 30 mM glucose, with or without fidarestat (10 μM) for 3-14 days. Apoptosis was assessed by TUNEL assay, nitrotyrosine and poly(ADP-ribose) by immunocytochemistry, and Bax and Bcl-2 expression by Western blot analyses. Fidarestat treatment prevented diabetic cataract formation and counteracted retinal nitrosative stress, and poly(ADP-ribose) polymerase activation, as well as glial activation. The number of TUNEL-positive nuclei (mean ± SEM) was increased approximately 4-fold in diabetic rats vs. controls (207±33 vs. 49±4, p<0.01), and this increase was partially prevented by fidarestat (106±34, p<0.05 vs. untreated diabetic group). The apoptotic cell number increased with the prolongation of exposure of both pericytes and endothelial cells to high glucose levels. Fidarestat counteracted nitrotyrosine and poly(ADP-ribose) accumulation and apoptosis in both cell types. Antiapoptotic effect of fidarestat in high glucose-exposed retinal pericytes was not associated with the inhibition of Bax or increase in Bcl-2 expression. In conclusion, the findings, i) support an important role for aldose reductase in diabetes-associated cataract formation, and retinal oxidative-nitrosative stress, glial activation, and apoptosis, and ii) provide a rationale for the development of aldose reductase inhibitors, and, in particular, fidarestat, for the prevention and treatment of diabetic ocular complications.

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Section: Discussionsupporting

confidence: 80%

Aldose reductase inhibitor fidarestat counteracts diabetes-associated cataract formation, retinal oxidative-nitrosative stress, glial activation, and apoptosis

Drel

Pacher²,

Ali³

et al. 2008

Int J Mol Med

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“…In particular, a 52-week multicenter (78 centers in Japan) placebo-controlled double-blind parallel group study of the AR inhibitor fidarestat in 279 patients with type 1 and type 2 diabetes and associated peripheral neuropathy revealed beneficial effects of treatment on subjective symptoms including numbness, spontaneous pain, sensation of rigidity, paresthesia in the sole upon walking, heaviness in the foot, and hypesthesia. 105 Similar results have been achieved in the 3-year, multicenter (112 centers in Japan), comparative Aldose Reductase InhibitorDiabetes Complications Trial in 594 subjects with diabetic neuropathy, in which numbness of limbs, sensory abnormalities, and cramping were alleviated in patients treated with the AR inhibitor epalrestat compared with the placebo group. 106 A more recent open-label pilot study (12 hospitals in Japan, 22 patients) revealed beneficial effect of fidarestat on vibration perception threshold of the upper and lower limbs and subjective symptoms of PDN, such as severity of numbness in the lower limbs, heaviness in the foot, coldness and hot flushes in the lower limbs, smarting pain causing difficulty in walking, sensation as if walking on sand, sensation as if walking on an uneven road, spontaneous pain in the lower limbs, and dizziness.…”

Section: Summary Of the Current Knowledge On The Key Mechanisms Of DIsupporting

confidence: 67%

“…35,36 Glutamate concentrations in the peripheral nerve system are reduced by AR inhibitor, 35 vasodilator, 122 and antioxidant 123 treatments-and all these treatments also alleviate symptoms of diabetic neuropathic pain in diabetic animal models 19,20 -22,77,78,99,102 and in human subjects. [105][106][107]111,112,114,124 Several reports indicate that the pro-inflammatory cytokine tumor necrosis factor alpha (TNF-␣) plays a role in nondiabetic painful neuropathy. [125][126][127] It is quite plausible that it also plays a role in diabetic neuropathic pain (as has been suggested 128,129 ), because TNF-␣ expression is increased in tissues of diabetic animals, and TNF-␣ induces overexpression of cyclooxygenase-2, 130,131 also implicated in diabetic hyperalgesia and allodynia.…”

Section: Strategies For Drug Discoverymentioning

confidence: 99%

Diabetic Painful and Insensate Neuropathy: Pathogenesis and Potential Treatments

2009

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Summary:Advanced peripheral diabetic neuropathy (PDN) is associated with elevated vibration and thermal perception thresholds that progress to sensory loss and degeneration of all fiber types in peripheral nerve. A considerable proportion of diabetic patients also describe abnormal sensations such as paresthesias, allodynia, hyperalgesia, and spontaneous pain. One or several manifestations of abnormal sensation and pain are described in all the diabetic rat and mouse models studied so far (i.e., streptozotocin-diabetic rats and mice, type 1 insulinopenic BB/Wor and type 2 hyperinsulinemic diabetic BBZDR/Wor rats, Zucker diabetic fatty rats, and nonobese diabetic, Akita, leptin-and leptin-receptor-deficient, and highfat diet-fed mice). Such manifestations are 1) thermal hyperalgesia, an equivalent of a clinical phenomenon described in early PDN; 2) thermal hypoalgesia, typically present in advanced PDN; 3) mechanical hyperalgesia, an equivalent of pain on pressure in early PDN; 4) mechanical hypoalgesia, an equivalent to the loss of sensitivity to mechanical noxious stimuli in advanced PDN; 5) tactile allodynia, a painful perception of a light touch; and 5) formalin-induced hyperalgesia. Rats with short-term diabetes develop painful neuropathy, whereas those with longer-term diabetes and diabetic mice typically display manifestations of both painful and insensate neuropathy, or insensate neuropathy only. Animal studies using pharmacological and genetic approaches revealed important roles of increased aldose reductase, protein kinase C, and poly(ADPribose) polymerase activities, advanced glycation end-products and their receptors, oxidative-nitrosative stress, growth factor imbalances, and C-peptide deficiency in both painful and insensate neuropathy. This review describes recent achievements in studying the pathogenesis of diabetic neuropathic pain and sensory disorders in diabetic animal models and developing potential pathogenetic treatments. Key Words: Animal models, diabetic insensate neuropathy, diabetic painful neuropathy, formalin-induced hyperalgesia, mechanical hyper-and hypoalgesia, pathogenetic treatments of diabetic neuropathic pain and sensory loss, symptomatic treatments of diabetic pain, tactile allodynia, thermal hyper-and hypoalgesia.

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“…Our data showed significant effects on both NO and NBF. A previous study reported that fidarestat had stronger aldose reductase inhibition and longer half-life in the peripheral nerve than other ARIs [32]. These points could explain why fidarestat is more effective on NO and NBF in improving conduction velocity.…”

Section: Discussionmentioning

confidence: 81%

“…Fidarestat is active in several sites of action. It is a powerful ARI and reduces polyol accumulation [32]. The other mechanism is the polyol pathway being active in the endothelial cell.…”

Section: Discussionmentioning

confidence: 99%

Effect of the aldose reductase inhibitor fidarestat on experimental diabetic neuropathy in the rat

Kuzumoto

Kusunoki

Kato³

et al. 2006

Diabetologia

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Aims/hypothesis Fidarestat, an aldose reductase inhibitor (ARI), has been reported to improve clinical symptoms and nerve conduction deficits in human diabetic neuropathy. We evaluated the dose-dependency and some of the mechanisms of the drug action in experimental diabetic neuropathy (EDN). Methods Control rats and rats with EDN were fed on normal pellets or pellets containing 0.00066% (1 mg/kg) or 0.00263% (4 mg/kg) fidarestat for 10 weeks. We evaluated the effect of fidarestat on nerve blood flow (NBF), electrophysiology, and sorbitol and fructose content in sciatic nerve in control and diabetic rats. For detection of oxidative stress in peripheral nerve, we measured sciatic nerve reduced glutathione (GSH) and 8-hydroxy-2′-deoxyguanosine (8-OHdG) immunolabelling of dorsal root ganglion (DRG) neurons. Results NBF, compound muscle action potential and amplitude of C-potential were significantly improved in diabetic rats fed on the diet supplemented with fidarestat. Fidarestat suppressed the increase in sorbitol and fructose, normalised GSH in sciatic nerve, and reduced the number of 8-OHdG-positive cells in DRG. Conclusions/interpretation Fidarestat improves neuropathy, presumably via an improvement in oxidative stress. This study supports a role for fidarestat in the treatment of diabetic neuropathy.

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Clinical Efficacy of Fidarestat, a Novel Aldose Reductase Inhibitor, for Diabetic Peripheral Neuropathy

Cited by 205 publications

References 27 publications

Aldose reductase inhibitor fidarestat counteracts diabetes-associated cataract formation, retinal oxidative-nitrosative stress, glial activation, and apoptosis

Aldose reductase inhibitor fidarestat counteracts diabetes-associated cataract formation, retinal oxidative-nitrosative stress, glial activation, and apoptosis

Diabetic Painful and Insensate Neuropathy: Pathogenesis and Potential Treatments

Effect of the aldose reductase inhibitor fidarestat on experimental diabetic neuropathy in the rat

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