Glucose Tolerance and Insulin Release in Malnourished Rats

Weinkove, C.; Weinkove, E.; Pimstone, B. L.

doi:10.1042/cs0500153

Cited by 26 publications

(32 citation statements)

References 31 publications

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“…Several previous investigations have failed to demonstrate a protein-losing catabolic state in malignant cachexia (Waterhouse et al, 1951;Fenninger and Mider, 1954;Holroyde et al, 1975 (Sherman et al, 1950). Evidently, protein deprivation in advanced cancer seems to arise not only from anorexia, the major cause of cachexia (Theologides, 1972) but also from monopolization of the host's protein metabolic pool by the tumour tissue (Mider et al, 1948 (Weinkove et al, 1976). This fact, taken in conjunction with our data on glucagon-mediated insulin release in cachectic cancer patients, suggests a similar underlying mechanism for glucose intolerance in human neoplasia.…”

Section: Discussionsupporting

confidence: 75%

“…Recent studies on malnourished children (Milner, 1971), adults (Smith et al, 1975) and animals (Heard, 1966;Weinkove et al, 1976) conclusively demonstrate that malnutrition can lead to glucose intolerance. In particular the work on malnourished animals (Weinkove et al, 1976) has implicated protein deficiency as an important precursor of impaired carbohydrate metabolism.…”

mentioning

confidence: 99%

“…In particular the work on malnourished animals (Weinkove et al, 1976) has implicated protein deficiency as an important precursor of impaired carbohydrate metabolism. For instance, weanling rats fed a protein-deficient diet and challenged with i.v.…”

mentioning

confidence: 99%

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Mechanism of impaired glucose tolerance in patients with neoplasia

Jasani¹,

Donaldson²,

Ratcliffe³

et al. 1978

Br J Cancer

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Summary.-The disappearance rate (k) of i.v. glucose was measured in cachectic and non-cachectic cancer patients and tumour-free controls. The respective k values were found to be 106+027 (mean+s.d.), 164±034 and 163±023. Of the other parameters measured, only plasma albumin level was found to vary significantly amongst the 3 categories, the mean level being the lowest in cachectic cancer patients. The means of total plasma protein, fasting blood glucose and plasma liver enzyme concentrations were similar in the 3 groups. Glucagon, a potent insulin secretogogue, failed to augment the fasting insulin level in cachectic but did so in non-cachectic cancer patients. Taken together, the findings suggest that the reduced glucose tolerance in patients with neoplasia is due to impairment of insulin release exhibited predominantly by ill-nourished advanced cancer patients having a moderate to severe degree of hypoalbuminemia.

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Section: Discussionsupporting

confidence: 75%

mentioning

confidence: 99%

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Mechanism of impaired glucose tolerance in patients with neoplasia

Jasani¹,

Donaldson²,

Ratcliffe³

et al. 1978

Br J Cancer

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“…The low basal insulin levels in kwashiorkor, and the impaired insulin reserve in kwashiorkor and marasmic-kwashiorkor patients can be attributed to the effect of their unbalanced high energy-low protein diet. In support of this view, in experimental animals maintained on low protein diets where the carbohydrate content is necessarily high, plasma insulin levels are consistently low (54,55).…”

Section: Discussionmentioning

confidence: 63%

Serum Insulin-Like Growth Factors I and II Concentrations and Growth Hormone and Insulin Responses to Arginine Infusion in Children with Protein-Energy Malnutrition before and after Nutritional Rehabilitation

et al. 1986

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ABSTRACT. Serum insulin, growth hormone (GH), insulin-like growth factors (IGFs) I and 11, cortisol, and albumin concentrations were measured in 15 children with kwashiorkor, 15 with marasmic-kwashiorkor, and 21 with marasmus, before and in the survivors, after nutritional rehabilitation, as well as in 10 underweight and eight normal Egyptian children. We also evaluated arginineinduced insulin and GH secretion. IGF-I concentrations were reduced in the three severely malnourished groups (0.07 2 0.03, 0.05 + 0.03, and 0.09 f 0.09 U/ml, respectively) but returned to normal after refeeding. IGF-I1 concentrations were low in the kwashiorkor (175 f 79 ng/ml), marasmic-kwashiorkor (1 11 2 57 ng/ml), and marasmic children (128 2 70.9 ng/ml) and returned to normal after nutritional rehabilitation. Basal GH levels were high in the three severely malnourished groups (21.9, 28.8, and 16.6 ng/ml, respectively) and returned to normal after refeeding (8.1, 6.5, and 6.0 ng/ml, respectively). GH responses to arginine were depressed in the three malnourished groups and improved significantly in marasmic-kwashiorkor and marasmic children after nutritional rehabilitation. Insulin responses to arginine were impaired in kwashiorkor, and marasmic-kwashiorkor children and improved significantly after refeeding. IGF-I levels correlated significantly with percent of expected weight ( r = 0.52, p < 0.001), percent of expected height ( r = 0.42, p < 0.001), and weight/ (height)' index ( r = 0 . 3 4 ,~ < 0.01). IGF-I levels correlated positively with insulin levels ( r = 0.421, p < 0.001) and negatively with cortisol concentrations ( r = -0.400, p <

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“…Seule une diminution de la riposte insulinique à une stimulation par le glucose est unanimement admise. Par contre, une controverse persiste à propos des répercussions de la malnutrition sur les réserves pancréatiques en insuline (Levine et al, 1983 ;Weinkove et al, 1976), sur la réponse des cellules B à d'autres stimuli que le glucose (Weinkove et a/., 1976 ;Younoszai and Dixit, 1980) et sur la sensibilité des tissus à l'action de l'insuline (Weinkove et al, 1976 ;Becker, 1983 …”

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