Peripheral neuropathy in mouse hereditary diabetes mellitus

Hanker, Jacob S.; Ambrose, Wallace W.; Yates, Peggy E.; Koch, Gary G.; Carson, Keith A.

doi:10.1007/bf00690457

Cited by 24 publications

(6 citation statements)

References 30 publications

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“…Animals with advanced diabetes also exhibited microangiopathic changes characterized by basement membrane thickening. This sequence of structural changes is similar to those reported in other spontaneously diabetic laboratory animals (Sima & Robertson, 1978a;Hanker et al, 1980;Yagihasi et al, 1981), and has led to the opinion that diabetic neuropathy is basically an axonal disorder (Jacobsen, 1976a;197613;Y agihashi et al, 1978;Sima & Robertson, 1979;Robertson & Sima, 1980;Sima, 1980aSima, , 1980bBrown et al, 1980). However, our knowledge concerning factors responsible for the development of nerve dysfunction in diabetes is scanty.…”

Section: Introductionsupporting

confidence: 77%

Functional Aspects and Pathogenetic Considerations of the Neuropathy in the Spontaneously Diabetic Bb‐wistar Rat

Sima

Hay

1981

Neuropathology Appl Neurobio

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Electrophysiological features were studied longitudinally in the spontaneously diabetic insulin-dependent, BB-Wistar rat. These were correlated in time with the state of the patency of the protective barriers in peripheral nerves. Motor nerve conduction velocity was significantly slowed only 3 weeks after the onset of the diabetes. When ultrastructural changes began, the maximal conduction velocity was further diminished. The amplitudes of evoked muscle potentials and distal latencies were significantly altered in diabetic rats. No change in the permeability of the blood-nerve barrier could be demonstrated before, during or after the onset of the nerve conduction defect. The possible pathogenetic mechanisms are discussed and a possible mechanism is suggested, namely a reduced availability of energy to axons in diabetes.

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Section: Introductionsupporting

confidence: 77%

Functional Aspects and Pathogenetic Considerations of the Neuropathy in the Spontaneously Diabetic Bb‐wistar Rat

Sima

Hay

1981

Neuropathology Appl Neurobio

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“…Alterations in pancreatic (Coleman, 19781, renal (Like et al, 1972), CNS (Garris et al, 1985a,b), peripheral nerve (Hanker et al, 1980), and hepatic (Coleman, 1982) structure and function are recognized to occur in association with the diabetes syndrome in this murine model. The changes are influenced by the duration of the hyperglycemic-hyperinsulinemic condition that characterizes the expression of the genetic mutation in this murine model.…”

Section: Discussionmentioning

confidence: 83%

Ultrastructural and metabolic changes associated with reproductive tract atrophy and adiposity in diabetic female mice

1986

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The effect of progressive, diabetes-associated adiposity on reproductive tract structure and function was examined in 4- to 16-week-old C57BL/KsJ, control (+/?) and diabetic (db/db) mice. Uterine and ovarian tissues were analyzed by transmission electron microscopy for ultrastructural changes associated with increased intracellular lipid accumulation. In addition, the same tissues were analyzed for changes in activity of tissue lipoprotein lipase, an enzyme that hydrolyzes lipoprotein-associated triacylglycerols and supports the cellular uptake and storage of free fatty acids. Between 8 and 16 weeks of age, intracellular lipid deposits increased dramatically in the ovarian granulosa, thecal and stromal cell populations, as well as in the uterine epithelium, of diabetic mice compared to controls. By 16 weeks of age, the lipid deposits essentially occupied the entire cytoplasmic area of both the ovarian and uterine cell types in diabetics. The basal lamina underlying the uterine epithelium was expanded in the diabetics relative to controls, and the hyperglycemic condition induced an observable increase in endometrial intercellular space that was occupied by a hyaline type of ground substance of unknown composition and origin. In association with these structural changes, both ovarian and uterine lipase activities were greatly increased in the db/db mice compared with controls. These data suggest that the structural adiposity and functional decline in reproductive tract condition of the db/db mutants are related to the enhanced cellular lipid deposition observed in this species. These changes in structural and metabolic parameters are related to the reproductive incompetence characteristic of this murine model.

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“…Although the present studies focused on the intracellular structural and functional parameters modified by the diabetes-obesity syndrome in (dbldb) mice, similar cellular changes may relate to alterations in pancreatic, renal, hepatic and CNS tissue function in this model (Barlett and Garris, 1987;Bower et al, 1980;Bray and York, 1979;Coleman, 1967Coleman, ,1978Coleman, ,1982Garris, 1984aGarris, , 1987aGarris et al, 1984aGarris et al, ,b, 1985aGarris and Michel, 1988;Gartner, 1979;Hanker et al, 1980;Herberg and Coleman, 1977;Johnson and Sidman, 1979;Like et al, 1974;Meade et al, 1981;Moore et al, 1980;Sima and Robertson, 1979). Regardless of the particular tissue, the longer the diabetic condition persists, the more pronounced and dramatic are the cellular alterations in this animal model.…”

Section: Discussionmentioning

confidence: 95%

“…Alterations in follicular growth and recruitment patterns, ovarian steroid production, corpus luteum formation, cellular and interstitial structure, uterine epithelial activity, endometrial sensitivity to exogenous steroid therapy, and ovarian refractoriness to pituitary gonadotrophin stimulation are well-recognized consequences of the diabetes-obesity syndrome in this mutant mouse model (Barlett and Garris, 1987;Coleman, 1967;Garris, 1985Garris, , 1987bJohnson and Sidman, 1979;Garris et al, 1984aGarris et al, ,b, 1985aGarris et al, -c, 1986. In addition, the accompanying changes in pancreatic, hepatic, renal, neuronal, and peripheral nerve structure and function are associated with the expression of the altered carbohydrate metabolism and imbalanced glucose homeostasis, characterized by overt hyperglycemia and hyperinsulinemia [Bower et al, 1980;Bray and York, 1979;Coleman, 1967Coleman, , 1978Coleman, , 1982Garris et al, 1985a-c, Gartner, 1979Hanker et al, 1980;Like et al, 1974;Meade et al, 1981;Moore et al, 1980;Sima and Robertson, 1979). Changes in cellular glucose uptake rates (Garris et al, 1984a(Garris et al, ,b, 1985aGarris and Michel, 1988), as well as noradrenergic counterregulatory influences (Garris, 1988b1, exacerbate the diabetes-associated depression in intercellular processing, responsivity , sensitivity, structure, and function (Garris, 1985;Garris et al, 1985aGarris et al, -q 1986.…”

mentioning

confidence: 99%

Effects of estradiol and progesterone on diabetes‐associated utero‐ovarian atrophy in C57BL/KsJ (db/db) mutant mice

Garris

1989

Anat. Rec.

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The modulating effects of estradiol (E: 1 microgram/3.5 days) and progesterone (P: 2 mg/3.5 days) on the obesity and hyperinsulinemic and hyperglycemic components of the diabetes-obesity syndrome in female C57BL/KsJ (db/db) mice, which includes cellular atrophy and adiposity in the reproductive tract, were examined and compared to corresponding control (+/?) parameters. All control and diabetic mice received oil (vehicle control), E, or P treatments starting at 4 weeks of age. Body weight, serum insulin levels, blood glucose concentrations, and utero-ovarian lipoprotein lipase activities were analyzed at 8 and 16 weeks of age and related to the ultrastructural changes in the steroid-sensitive uterine epithelium during the treatment period. Neither E nor P had any effect on body weights in (+/?) or (db/db) mice. The pronounced diabetes-associated elevation in serum insulin levels was enhanced by E, and suppressed by P, in 16-week-old (db/db) mice as compared with controls. By 16 weeks of age, the E therapy normalized blood glucose levels in diabetic mice to control levels, whereas P was ineffective in modulating the hyperglycemia. The reduction in blood glucose levels in E-treated diabetic mice correlated temporally with the return of normal intracellular structure including the disappearance of intracellular lipid vacuoles characteristic of uterine epithelium cells of (db/db) mice. The diabetes-induced rise in utero-ovarian lipoprotein lipase activity was normalized by P-therapy. The reduction in utero-ovarian lipoprotein lipase activity coincided temporally with the demonstrated intracellular reorganization in (db/db) reproductive tract tissues.(ABSTRACT TRUNCATED AT 250 WORDS)

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Peripheral neuropathy in mouse hereditary diabetes mellitus

Cited by 24 publications

References 30 publications

Functional Aspects and Pathogenetic Considerations of the Neuropathy in the Spontaneously Diabetic Bb‐wistar Rat

Functional Aspects and Pathogenetic Considerations of the Neuropathy in the Spontaneously Diabetic Bb‐wistar Rat

Ultrastructural and metabolic changes associated with reproductive tract atrophy and adiposity in diabetic female mice

Effects of estradiol and progesterone on diabetes‐associated utero‐ovarian atrophy in C57BL/KsJ (db/db) mutant mice

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