ZIB

1

Electronic Resource

Alerations of lymphocyte subsets in children of diabetic mothers (1994)

Roll, U. ; Scheeser, J. ; Standl, E. ; [et al.]

Springer

Diabetologia 37 (1994), S. 1132-1141

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ISSN: 1432-0428

Keywords: Lymphocyte subsets ; insulin-dependent diabetes mellitus ; gestational diabetes ; cord blood

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary To investigate the impact of diabetic mothers on the maturation of the immune system in their offspring, immunophenotypic markers of major lymphocyte subpopulations were evaluated by two-colour flow cytometric analysis in 160 healthy children of diabetic mothers (100 with insulin-dependent diabetes mellitus (IDDM); 48 with gestational diabetes), including 22 neonates, 45 infants aged 8–12 months, 46 children aged 1–2 years, 29 children aged 3–6 years and 18 children aged 7–17 years. Results were compared with 21 neonates of healthy mothers from our hospital and with 110 paediatric subjects of a reference population. In neonates of diabetic mothers, percentages of total lymphocytes (p=0.044), T and B lymphocytes (p=0.004, respectively) were significantly decreased compared to our neonates of healthy mothers. By subdividing the group of neonates in offspring of mothers with IDDM (n=15) or gestational diabetes (n=7), differences compared to normal neonates were mainly observed in neonates of mothers with IDDM (T lymphocytes: p=0.006; B lymphocytes: p=0.008). In cord blood, 45.5% of neonates had antibodies to islet cells, insulin or glutamic acid decarboxylase, most likely transmitted through the placenta of the diabetic mother. No association was found between alterations of lymphocyte subsets and antibody-positivity in cord blood, nor was there any correlation of lymphocyte counts and mean HbA1 during pregnancy, maternal age at delivery, diabetes duration, or neonatal birth weight, respectively. Comparisons among age groups from newborn infants through adolescents revealed higher percentages of total lymphocytes and lower percentages of activated T cells in children of diabetic mothers compared to children of the reference population between the age of 1 to 6 years (67–73% of the cases above and 62–77% below the interquartiles of the reference range, respectively). No significant differences in lymphocyte subpopulations between children of mothers with IDDM diabetes and gestational diabetes have been detected. In addition, there were no abnormalities of lymphocyte subsets in children who are at high risk for the development of IDDM. In summary, we suggest that the observed changes in children of diabetic mothers may reflect a cellular immune reaction to the particular maternal environment, characterized by both an abnormal metabolic state and persisting autoimmunity in the affected mother.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00418377

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2

Electronic Resource

Alterations of lymphocyte subsets in children of diabetic mothers (1994)

Roll, U. ; Scheeser, J. ; Standl, E. ; [et al.]

Springer

Diabetologia 37 (1994), S. 1132-1141

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ISSN: 1432-0428

Keywords: Key words Lymphocyte subsets ; insulin-dependent diabetes mellitus ; gestational diabetes ; cord blood.

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary To investigate the impact of diabetic mothers on the maturation of the immune system in their offspring, immunophenotypic markers of major lymphocyte subpopulations were evaluated by two-colour flow cytometric analysis in 160 healthy children of diabetic mothers (100 with insulin-dependent diabetes mellitus (IDDM); 48 with gestational diabetes), including 22 neonates, 45 infants aged 8–12 months, 46 children aged 1–2 years, 29 children aged 3–6 years and 18 children aged 7–17 years. Results were compared with 21 neonates of healthy mothers from our hospital and with 110 paediatric subjects of a reference population. In neonates of diabetic mothers, percentages of total lymphocytes (p = 0.044), T and B lymphocytes (p = 0.004, respectively) were significantly decreased compared to our neonates of healthy mothers. By subdividing the group of neonates in offspring of mothers with IDDM (n = 15) or gestational diabetes (n = 7), differences compared to normal neonates were mainly observed in neonates of mothers with IDDM (T lymphocytes: p = 0.006; B lymphocytes: p = 0.008). In cord blood, 45.5 % of neonates had antibodies to islet cells, insulin or glutamic acid decarboxylase, most likely transmitted through the placenta of the diabetic mother. No association was found between alterations of lymphocyte subsets and antibody-positivity in cord blood, nor was there any correlation of lymphocyte counts and mean HbA1 during pregnancy, maternal age at delivery, diabetes duration, or neonatal birth weight, respectively. Comparisons among age groups from newborn infants through adolescents revealed higher percentages of total lymphocytes and lower percentages of activated T cells in children of diabetic mothers compared to children of the reference population between the age of 1 to 6 years (67–73 % of the cases above and 62–77 % below the interquartiles of the reference range, respectively). No significant differences in lymphocyte subpopulations between children of mothers with IDDM diabetes and gestational diabetes have been detected. In addition, there were no abnormalities of lymphocyte subsets in children who are at high risk for the development of IDDM. In summary, we suggest that the observed changes in children of diabetic mothers may reflect a cellular immune reaction to the particular maternal environment, characterized by both an abnormal metabolic state and persisting autoimmunity in the affected mother. [Diabetologia (1994) 37: 1132–1141]

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00418377

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Peptide mapping and characterisation of glycation patterns of the glima 38 antigen recognised by autoantibodies in Type I diabetic patients (2000)

Roll, U. ; Turck, C. W. ; Gitelman, S. E. ; [et al.]

Springer

Diabetologia 43 (2000), S. 598-608

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ISSN: 1432-0428

Keywords: Keywords Type I diabetes ; immunology ; autoantibodies ; target autoantigen ; 38 000 Mr autoantigen ; glima 38 ; proteolytic cleavage ; peptide mapping ; lectin binding ; deglycation.

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Aims/hypothesis. Glima 38 is an N-glycated neuroendocrine membrane protein of Mr 38 000, which is recognised by autoantibodies in approximately 20 % of patients with Type I (insulin-dependent) diabetes mellitus. The aim of this study was to characterise the carbohydrate moiety and generate peptide maps of glima 38. Methods. Sera of high immunoreactivity to glima 38 were used to isolate 35-S methionine-labelled protein from βTC-3 cells and a neuronal cell line GT1.7. Tunicamycin was used to inhibit N-glycation of glima 38 and define the core protein. The carbohydrate moiety was characterised for tunicamycin sensitivity, lectin binding and susceptibility to different endoglycosidases. The protein moiety was subjected to digestion by proteases to define peptide maps. Results. The autoreactive epitopes in glima 38 recognised by Type I diabetic sera are conformational and independent of the carbohydrate moiety. Inhibition of N-glycation of glima 38 in vivo, shows a protein core of Mr 22 000 in both pancreatic β-(βTC3) and neuronal (GT1.7) cell lines. The carbohydrate moieties in the two cell types are distinct but contain a similar amount of terminal sialic acid residues and at least five oligosaccharide chains Glima 38 binds Triticum vulgare and Ricinus communis I lectins. Endoproteinase treatment of the Mr 22 000 core protein results in peptides of Mr 4500 and Mr 20 000 with Lys-C, and peptides of Mr 4 000 and Mr 11 000–12 000 with Glu-C/V8 and Asp-N proteases. Conclusion/interpretation. The biochemical properties of glima 38 define it as a new autoantigen in Type I diabetes and provide a basis for its purification. [Diabetologia (2000) 43: 598–608]

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s001250051349

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4

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Metal-ligand and π singlet-triplet transitions in phthalocyanine films studied by inelastic electron tunneling spectroscopy

Roll, U. ; Ewert, S. ; Luth, H.

Amsterdam : Elsevier

Chemical Physics Letters 58 (1978), S. 91-94

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ISSN: 0009-2614

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Chemistry and Pharmacology , Physics

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0009-2614(78)80323-6

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5

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L-pilin variants of Neisseria gonorrhoeae MS11 (1991)

Manning, P. A. ; Kaufmann, A. ; Roll, U. ; [et al.]

Oxford, UK : Blackwell Publishing Ltd

Molecular microbiology 5 (1991), S. 0

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ISSN: 1365-2958

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Biology , Medicine

Notes: Phase- and antigenic variation of pilin expression in Neisseria gonorrhoeae is based on the genetic exchange between silent pilin genes (pilS)and the pilin expression locus (pilE). Similarly, the non-piliated L-variants of strain MS11, which show an increased resistance to certain antibiotics, are the result of recombination with the pilElocus. However, this recombination is atypical in that pilE(L) carries a tandem arrangement of a complete pilin gene and additional partial pilin genes under the control of the same pilE promoter. Since the two pilin gene copies are tandemly arranged and are often in the same translational frame, oversized pilin molecules are produced, which do not assemble into pili. The tandem gene copies introduced in a piiE(L)locus originate from silent loci where they are already joint. Upon reversion to the P+ phenotype the L-variants lose one pilin gene copy from the pilE(L) in a process reminiscent of the deletion events that otherwise lead to the formation of the non-revertible and non-piliated Pn mutants of MS11 gonococci. Thus deletion of pilin genes from pHE can be regarded as a third mechanism of pilin variation in gonococci.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1365-2958.1991.tb00766.x

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6

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Ultra thin film sputter depth profiling (1999)

Moulder, J. F. ; Bryan, S. R. ; Roll, U.

Springer

Fresenius' journal of analytical chemistry 365 (1999), S. 83-84

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ISSN: 1432-1130

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract As semiconductor device geometry continues to shrink, new ultra thin material systems are developed. One such structure is a thin silicon oxy-nitride (ONO) film used in memory devices. Secondary Ion Mass Spectrometry (SIMS), because of its extreme surface sensitivity (small sampling depth), is routinely used to study thin ONO structures. However, interpretation and quantification of SIMS data is often difficult because of matrix effects that impact the secondary ion yield of different chemical species. With the Quantum 2000 Scanning ESCA MicroprobeTM, it is possible to obtain surface sensitivity equivalent to SIMS, using a low (20°) photoelectron take-off angle. The resulting ESCA data contain quantitative chemical state information that is difficult to obtain by other methods.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s002160051449

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7

Electronic Resource

Passivschichten auf rostfreien Stählen: Eine Übersicht über oberflächenanalytische Ergebnisse (1984)

Fischmeister, H. ; Roll, U.

Springer

Fresenius' Zeitschrift für analytische Chemie 319 (1984), S. 639-645

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ISSN: 1618-2650

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Description / Table of Contents: Zusammenfassung Rostfreie Stähle werden durch dünne Oxy-Hydroxidschichten passiviert, die gegenüber der Legierung stark an Chrom angereichert sind. Nach einem Jahrzehnt oberflächenanalytischer Forschung zeichnet sich eine Konvergenz der Ergebnisse ab, aus der einige verallgemeinernde Schlußfolgerungen abgeleitet werden können. Die Schichtdicke wächst linear mit dem Potential; das elektrische Feld in der Schicht und ihr Hydroxylgehalt scheinen von ihrem Chromgehalt bestimmt zu sein. Die Oxidschichten sind nur dann dauerhaft stabil, wenn sie mehr als 50% Cr enthalten. Der stationäre Wert der Cr-Anreicherung im Film und die Kinetik des Anreicherungsverlaufes können mit Hilfe eines Modells quantitativ beschrieben werden, das auf der Annahme präferentieller Auflösung von Eisen gegenüber Chrom (in einem konstanten Verhältnis von ca. 8∶1) beruht. Die Rolle des Nickels und des Molybdäns für die verbesserte Passivierbarkeit der Chromstähle wird qualitativ erörtert.

Notes: Summary Stainless steels are passivated by formation of a thin layer of oxy-hydroxide strongly enriched in chromium. A decade of surface analytical research has yielded converging results from which some generalized conclusions can be derived. The thickness of the films increases linearly with the potential; both the hydroxyl content and the electric field across the film appear to be linearly related to its chromium/iron ratio. Oxide films containing less than 50% Cr do not seem to be permanently stable. Both the stationary value of the chromium enrichment in the film and the kinetics of the enrichment process can be quantitatively described by a model based on preferential dissolution of iron in the electrolyte at ca. eight times the rate of chromium dissolution. The roles of nickel and chromium in enhancing passivity are discussed in qualitative terms.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01226742

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