Diabetic peripheral neuropathy: evidence for apoptosis and associated mitochondrial dysfunction.

Srinivasan, Shanthi; Stevens, Martin J.; Wiley, John W.

doi:10.2337/diabetes.49.11.1932

Cited by 242 publications

(222 citation statements)

References 31 publications

(38 reference statements)

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“…An area of controversy is whether classical apoptosis in the peripheral nervous system is responsible for the neuropathic deficits observed in both animal models and human patients. Multiple studies report activation of caspases in DRG neurons both in vitro and in vivo (Russell et al, 1999;Srinivasan et al, 2000;Kishi et al, 2002;Russell et al, 2002;Cheng and Zochodne, 2003;Schmeichel et al, 2003;. Others detect some loss of DRG (Russell et al, 1999;Zochodne et al, 2001;Kishi et al, 2002) and in particular there is a statistically significant loss of large DRG neurons (Kishi et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

“…These ROS are associated with membrane lipid peroxidation, nitration of proteins and DNA damage (for review see (Vincent and Feldman, 2004). Mitochondrial oxidative injury coupled with loss of insulin and neurotrophic support contributes to mitochondrial inner membrane depolarization in sensory neurons, ballooning of mitochondria, release of cytochrome c into the cytosol, and activation of caspases in DRG neurons Schmeichel et al, 2003Srinivasan et al, 2000Cheng and Zochodne, 2003; all of which are associated with neuronal or axonal injury (Sasaki et al, 1997;Fujimura et al, 1999;Russell et al, 1999;Kishi et al, 2002;Huang et al, 2003). In the current study, both DRG neurons and SC show evidence of caspase activation and positive TUNEL labeling.…”

Section: Discussionmentioning

confidence: 99%

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Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Russell

Berent-Spillson

Vincent

et al. 2008

Neurobiology of Disease

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Clinical studies suggest that impaired glucose tolerance (IGT) is associated with the development of neuropathy. The aim of the current study was to determine if neuropathy developed in the female Zucker Diabetic Fatty (ZDF) rat, an animal model of IGT and type 2 diabetes. The ZDF rat develops impaired glucose tolerance (IGT) when fed a control diet, and frank diabetes when fed a high fat diet. Following 10 weeks of hyperglycemia, sensory nerve action potentials (SNAP) and compound motor action potentials (CMAP) were reduced and sensory conduction velocities were slowed (distal > proximal) in the tail and hind limb in ZDF animals with IGT and frank diabetes (p<0.01). Neuropathy was coupled with evidence of increased reactive oxygen species (ROS) and cellular injury in dorsal root ganglion (DRG) neurons from IGT animals. Our study supports the hypothesis that neuropathy develops in an animal model of IGT and is associated with evidence of oxidative injury in DRG and peripheral nerves.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Russell

Berent-Spillson

Vincent

et al. 2008

Neurobiology of Disease

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“…7B, C). To determine the mechanisms involved in insulin loss following STZ administration, β-cells apoptosis was assessed by a combination of TUNEL staining 19 with cleaved caspase-3 immunocytochemistry. GDNF-tg mice showed 4 fold less β-cell apoptosis than WT mice twelve days after injection with STZ as evidenced by the smaller number of TUNEL and cleaved caspase-3 positive β-cells in these mice (P<0.05; Fig.…”

Section: Gdnf Transgenic Are Resistant To the Induction Of Diabetes Mmentioning

confidence: 99%

Glial Cell Line-Derived Neurotrophic Factor Increases β-Cell Mass and Improves Glucose Tolerance

et al. 2008

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“…Explant cultures were grown by placing whole DRG onto collagen-coated 6-well culture dishes. Cultures were grown for 3 days in Neurobasal Medium containing 25 mM glucose (optimal basal glucose for neurons) (Russell et al, 1999;Russell et al, 2002;Srinivasan et al, 2000), with 0.5% B27 without antioxidants, 10 ng/ml Nerve Growth Factor, 0.5% Pen/Strep/Neo, and 0.7 mM l-glutamine, and 40 µM FUDR. Media was changed every 48 hours, and immediately before drug treatment.…”

Section: Cell Culturementioning

confidence: 99%

“…Despite the significant pathology associated with nerve degeneration, the etiology of neuropathy is still unclear. Several pathways have been suggested to be associated with glucose neurotoxicity (Tomlinson and Gardiner 2008) and diabetic neuropathy, for example oxidative stress (Cameron et al, 1993;Coppey et al, 2001;Obrosova et al, 2005;Pop-Busui et al, 2006;Russell et al, 2002), altered polyol metabolism (Cameron and Cotter 1997), mitochondrial dysfunction (Huang et al, 2003a;Montal, 1998;Russell et al, 2002), activation of certain cysteine proteases (caspases) (Russell et al, 1999;Srinivasan et al, 2000) (Cheng and Zochodne 2003;Schmeichel et al, 2003), and regulation of growth factors and their intermediate signaling pathways (Sayers et al, 2003;Tomlinson et al, 1996). However, the role of cytokines such as transforming growth factor β (TGF-β) in development of diabetic neuropathy is not clearly defined.…”

Section: Introductionmentioning

confidence: 99%

Transforming growth factor-β induces cellular injury in experimental diabetic neuropathy

Anjaneyulu

Berent-Spillson

Inoue

et al. 2008

Experimental Neurology

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The mechanism/s leading to diabetic neuropathy are complex. Transforming growth factor-β1 (TGF-β1) has been associated with diabetic nephropathy and retinopathy but not neuropathy. In this study, changes in TGF-β isoforms were examined in-vivo and in-vitro. Two groups of animals, streptozotocin diabetic with neuropathy and non-diabetic controls were examined at 4 weeks (n=10/ group) and 12 weeks (n=8/group). In diabetic DRG using quantitative real-time PCR (QRT-PCR), TGF-β1 and TGF-β2 mRNA, but not TGF-β3, was increased at 4 and 12 weeks. In sciatic nerve TGF-β3 mRNA was primarily increased. Immunohistochemistry (DRG) and immunoblotting (sciatic nerve) showed similar differential protein expression. In sciatic nerve TGF-β formed homoand heterodimers, of which β 2 /β 3 , β 1 /β 1 , and β 1 /β 3 were significantly increased, while that of the TGF-β 2 /β 2 homodimer was decreased, in diabetic compared to non-diabetic rats. In-vitro, pretreatment of embryonic DRG with TGF-β neutralizing antibody prevents the increase in total TGF-β protein observed with high glucose using immunoblotting. In high glucose conditions, combination with TGF-β2 > β1 increases the percent of cleaved caspase-3 compared to high glucose alone and TGF-β neutralizing antibody inhibits this increase. Furthermore, consistent with the findings in diabetic DRG and nerve, TGF-β isoforms applied directly in vitro reduce neurite outgrowth, and this effect is partially reversed by TGF-β neutralizing antibody. These findings implicate upregulation of TGF-β in experimental diabetic peripheral neuropathy and indicate a novel mechanism of cellular injury related to elevated glucose levels. In combination, these findings indicate a potential new target for treatment of diabetic peripheral neuropathy.

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Diabetic peripheral neuropathy: evidence for apoptosis and associated mitochondrial dysfunction.

Cited by 242 publications

References 31 publications

Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Glial Cell Line-Derived Neurotrophic Factor Increases β-Cell Mass and Improves Glucose Tolerance

Transforming growth factor-β induces cellular injury in experimental diabetic neuropathy

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