Mary Ann Morris scite author profile

Use of an ion exchange chromatographic method and a calorimetric method with thiobarbituric acid showed that levels of nonenzymatically glucosylated serum albumin were increased in patients with poorly controlled diabetes mellitus compared to controls. The two methods correlated well (r = 0.99) and clearly discriminated between normal and poorly controlled diabetic populations. The levels of glycosylated hemoglobin were also measured in both populations.Several patients apparently in good control based on glycosylated hemoglobin measurements were found to have increased levels of glucosylated albumin. Because albumin has a shorter circulating half-life than does the human erythrocyte, the plasma concentration of glucosylated albumin should be expected to reflect short-term control of hyperglycemia in diabetes. The studies reported here suggest that the level of glucosylated albumin may indeed be a sensitive indicator of moderate hyperglycemia and of early glucose intolerance. Recent studies showed that plasma proteins are glucosylated nonenzymatically by glucose in vitro (1). Glucosylated albumin was isolated from normal human serum by chromatography on CM-cellulose and accounted for about 8% of the total circulating albumin in man. The nonenzymatic glucosylation of albumin appears to proceed through Schiff base formation between the aldehyde form of the sugar and free amino groups in protein, followed by Amadori rearrangement to a ketoamine derivative (Fig.

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Pitt-Hopkins Syndrome: A Review of Current Literature, Clinical Approach, and 23-Patient Case Series

Goodspeed

Newsom

Morris³

et al. 2018

J Child Neurol

105

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Pitt-Hopkins syndrome (PTHS) is a rare, genetic disorder caused by a molecular variant of TCF4 which is involved in embryologic neuronal differentiation. PTHS is characterized by syndromic facies, psychomotor delay, and intellectual disability. Other associated features include early-onset myopia, seizures, constipation, and hyperventilation-apneic spells. Many also meet criteria for autism spectrum disorder. Here the authors present a series of 23 PTHS patients with molecularly confirmed TCF4 variants and describe 3 unique individuals. The first carries a small deletion but does not exhibit the typical facial features nor the typical pattern of developmental delay. The second exhibits typical facial features, but has attained more advanced motor and verbal skills than other reported cases to date. The third displays typical features of PTHS, however inherited a large chromosomal duplication involving TCF4 from his unaffected father with somatic mosaicism. To the authors' knowledge, this is the first chromosomal duplication case reported to date.

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Increased Circulating Ia-Antigen-Bearing T Cells in Type I Diabetes Mellitus

et al. 1982

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Differential Sensitivity to β-Cell Secretagogues in “Early,” Type I Diabetes Mellitus

Ganda¹,

Srikanta

Brink

et al. 1984

108

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The insulin secretory response to various beta-cell secretagogues was studied in four children (ages 11, 11, 12, and 10 yr) in "early" stages or remission of type I diabetes mellitus. One child was an anti-islet antibody positive monozygotic twin of a type I diabetic subject, two children had impaired glucose tolerance and elevated levels of Ia-positive T-cells, and the fourth was in remission (off insulin) of type I diabetes 6 mo after immunotherapy. The peak first-phase (0-10 min) insulin increment after intravenous (i.v.) glucose was negligible in each patient, whereas the peak responses to i.v. glucagon, tolbutamide, arginine, and oral glucose ranged between 10% and 43% of median responses in normal control subjects. The rank order of response to a variety of secretagogues was remarkably similar in all four subjects: i.v. arginine greater than i.v. glucagon greater than oral glucose greater than i.v. tolbutamide greater than i.v. glucose. These studies indicate that a "functional" beta-cell defect, namely a complete loss of response to i.v. glucose and a partial loss to other secretagogues, exists in type I diabetic patients before complete beta-cell destruction. This alteration in beta-cell responsiveness probably underlies our prior observation of slowly progressive loss of i.v.-glucose-induced insulin release in islet cell antibody-positive siblings to type I diabetic subjects.

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Mary Ann Morris

Enhanced nonenzymatic glucosylation of human serum albumin in diabetes mellitus.

Pitt-Hopkins Syndrome: A Review of Current Literature, Clinical Approach, and 23-Patient Case Series

Increased Circulating Ia-Antigen-Bearing T Cells in Type I Diabetes Mellitus

Differential Sensitivity to β-Cell Secretagogues in “Early,” Type I Diabetes Mellitus

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