Your search keyword '"Gallwitz, B"' showing total 19 results

1. Diabetes mellitus an der Schnittstelle von Pädiatrie und Erwachsenenmedizin.

Author

Gallwitz, B. and Neu, A.

Abstract

Copyright of Der Internist is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

2. Rezeptoragonisten des 'glucagon-like peptide 1'.

Author

Gallwitz, B.

Abstract

Copyright of Der Diabetologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2017

3. Physiology and Pathophysiology of Endocrine Pancreatic Secretion.

Author

Beger, Hans G., Matsuno, Seiki, Cameron, John L., Rau, Bettina M., Sunamura, Makoto, Schulick, Richard D., Gallwitz, B., and Fölsch, U. R.

Published

2008

4. Neue antihyperglykämische Therapeutika.

Author

Gallwitz, B. and Nitschmann, S.

Published

2014

5. Inkretinbasierte Therapien.

Author

Gallwitz, B.

Abstract

Copyright of Der Diabetologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013

6. Gemeinsamkeiten und Unterschiede inkretinbasierter Therapien.

Author

Gallwitz, B.

Abstract

Copyright of Der Diabetologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2011

7. Benefit-risk assessment of exenatide in the therapy of type 2 diabetes mellitus.

Author

Gallwitz B and Gallwitz, Baptist

Abstract

Exenatide is the first incretin mimetic, introduced into type 2 diabetes mellitus therapy in 2005, with first approval in the US. It is a glucagon-like peptide-1 (GLP-1) receptor agonist that can be used for treatment by twice-daily injection. A long-acting release formulation for once-weekly injection is in clinical development. Clinical studies and postmarketing experience with exenatide have shown a significant and sustained reduction in glycosylated haemoglobin (HbA(1c)) by approximately 1% together with other gylcaemic parameters without an intrinsic risk for hypoglycaemias, and a reduction in bodyweight by 5.3 kg in 82 weeks. Blood pressure and lipids are also favourably affected, but hard cardiovascular endpoints are not yet available. Animal studies show an improvement of beta-cell function and an increase in beta-cell mass after exenatide treatment. The most frequent adverse events associated with exenatide therapy are nausea and antibody formation (both approximately 40%). Nausea, mostly mild and transient, was responsible for a 6% dropout rate in clinical studies. A recent review on the association of acute pancreatitis with exenatide treatment showed no increased risk (relative risk 1.0; 95% CI 0.6, 1.7). This review gives a benefit-risk assessment of exenatide. [ABSTRACT FROM AUTHOR]

Published

2010

8. A common genetic variant in WFS1 determines impaired glucagon-like peptide-1-induced insulin secretion.

Author

Schäfer, S., Müssig, K., Staiger, H., Machicao, F., Stefan, N., Gallwitz, B., Häring, H., and Fritsche, A.

Abstract

WFS1 type 2 diabetes risk variants appear to be associated with impaired beta cell function, although it is unclear whether insulin secretion is affected directly or secondarily via alteration of insulin sensitivity. We aimed to investigate the effect of a common WFS1 single-nucleotide polymorphism on several aspects of insulin secretion. A total of 1,578 non-diabetic individuals (534 men and 1,044 women, aged 40 ± 13 years, BMI 28.9 ± 8.2 kg/m2 [mean ± SD]) at increased risk of type 2 diabetes were genotyped for rs10010131 within the WFS1 gene. All participants underwent an OGTT (and a subset additionally an IVGTT [ n = 319]) and a hyperglycaemic clamp combined with glucagon-like peptide-1 (GLP-1) and arginine stimuli ( n = 102). rs10010131 was associated with reduced OGTT-derived insulin secretion ( p = 0.03). In contrast, insulin secretion induced by an i.v. glucose challenge in the IVGTT and hyperglycaemic clamp was not different between the genotypes. GLP-1 infusion combined with a hyperglycaemic clamp showed a significant reduction of the insulin secretion rate during the first and second phases of GLP-1-induced insulin secretion in carriers of the risk allele (reduction of 36% and 26%, respectively; p = 0.007 and p = 0.04, respectively). A common genetic variant in WFS1 specifically impairs GLP-1-induced insulin secretion independently of insulin sensitivity. This defect might explain the impaired insulin secretion in carriers of the risk allele and confer the increased risk of type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2009

9. The risk allele load accelerates the age-dependent decline in beta cell function.

Author

Haupt, A., Staiger, H., Schäfer, S., Kirchhoff, K., Guthoff, M., Machicao, F., Gallwitz, B., Stefan, N., Häring, H.-U., and Fritsche, A.

Abstract

Among the novel type 2 diabetes risk loci identified by genome-wide association studies, TCF7L2, HHEX, SLC30A8 and CDKAL1 appear to affect beta cell function. In the present study we examined the effect of these genes’ risk alleles on the age-dependent decline in insulin secretion. The SNPs rs7903146 ( TCF7L2), rs7754840( CDKAL1), rs7923837 ( HHEX) and rs13266634 ( SLC30A8) were genotyped in 1,412 non-diabetic patients, who were subsequently grouped according to their number of risk alleles. All participants underwent an OGTT. Insulin secretion was assessed by validated indices and proinsulin conversion by calculating AUCproinsulin/AUCinsulin. The number of risk alleles revealed a Gaussian distribution, with most participants carrying four risk alleles. Stratification into groups with low (LAL, up to three alleles), median (MAL, four alleles) and high (HAL, five to eight alleles) allele load resulted in MAL and HAL participants displaying significantly lower insulin secretion and proinsulin conversion than LAL participants ( p ≤ 0.0014 and p = 0.0185, respectively). In the overall cohort, age was negatively associated with insulin secretion and proinsulin conversion (both p < 0.0001). MAL and HAL participants showed a significantly more pronounced decline in insulin secretion with increasing age than LAL participants ( p ≤ 0.0325; analysis of covariance), and after stratification for BMI this relationship was maintained in obese, but not non-obese, participants. Proinsulin conversion decreased with increasing age in MAL and HAL, but not LAL, participants ( p ≤ 0.0003 vs p = 0.2). The risk allele load significantly accelerates the age-dependent decline in beta cell function, and this might be of particular importance in obese people. [ABSTRACT FROM AUTHOR]

Published

2009

10. Impaired glucagon-like peptide-1-induced insulin secretion in carriers of transcription factor 7-like 2 ( TCF7L2) gene polymorphisms.

Author

Schäfer, S., Tschritter, O., Machicao, F., Thamer, C., Stefan, N., Gallwitz, B., Holst, J., Dekker, J., t’Hart, L., Nijpels, G., Haeften, T., Häring, H., and Fritsche, A.

Abstract

Polymorphisms in the transcription factor 7-like 2 ( TCF7L2) gene are associated with type 2 diabetes and reduced insulin secretion. The transcription factor TCF7L2 is an essential factor for glucagon-like peptide-1 (GLP-1) secretion from intestinal L cells. We studied whether a defect in the enteroinsular axis contributes to impaired insulin secretion in carriers of TCF7L2 polymorphisms. We genotyped 1,110 non-diabetic German participants for five single nucleotide polymorphisms in TCF7L2. All participants underwent an OGTT; GLP-1 secretion was measured in 155 participants. In 210 participants, an IVGTT combined with a hyperinsulinaemic–euglycaemic clamp was performed. In another 160 participants from the Netherlands and 73 from Germany, a hyperglycaemic clamp (10 mmol/l) was performed. In 73 German participants this clamp was combined with a GLP-1 infusion and an arginine bolus. The OGTT data confirmed that variants in TCF7L2 are associated with reduced insulin secretion. In contrast, insulin secretion induced by an i.v. glucose challenge in the IVGTT and hyperglycaemic clamp was not different between the genotypes. GLP-1 concentrations during the OGTT were not influenced by the TCF7L2 variants. However, GLP-1-infusion combined with a hyperglycaemic clamp showed a significant reduction in GLP-1-induced insulin secretion in carriers of the risk allele in two variants (rs7903146, rs12255372, p < 0.02). Variants of TCF7L2 specifically impair GLP-1-induced insulin secretion. This seems to be rather the result of a functional defect in the GLP-1 signalling in beta cells than a reduction in GLP-1 secretion. This defect might explain the impaired insulin secretion in carriers of the risk alleles and confers the increased risk of type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2007

11. Neue Substanzen in der oralen Medikation des Diabetes mellitus Typ 2.

Author

Gallwitz, B.

Abstract

Copyright of Der Diabetologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2007

12. Behandlungspfade in der Endokrinologie und Diabetologie.

Author

Gallwitz, B., Lehnert, H., Dittmann, H., Honegger, J., Teichmann, R., Tatagiba, M., and Häring, H.

Abstract

Copyright of Der Internist is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2006

13. Glucagon-like peptide 1 abolishes the postprandial rise in triglyceride concentrations and lowers levels of non-esterified fatty acids in humans.

Author

Meier, J. J., Gethmann, A., Götze, O., Gallwitz, B., Holst, J. J., Schmidt, W. E., and Nauck, M. A.

Subjects

GLUCAGON-like peptide 1, INSULIN, TRIGLYCERIDES, DIABETES, GASTROINTESTINAL hormones, PEPTIDE hormones

Abstract

Aims/hypothesis: Diabetic dyslipidaemia contributes to the excess morbidity and mortality in patients with type 2 diabetes. Exogenous glucagon-like peptide 1 (GLP-1) lowers postprandial glycaemia predominantly by slowing gastric emptying. Therefore, the effects of GLP-1 on postprandial lipid levels and gastric emptying were assessed. Methods: 14 healthy male volunteers were studied with an i.v. infusion of GLP-1 (1.2 pmol kg?1 min?1) or placebo over 390 min in the fasting state. A solid test meal was served and gastric emptying was determined using a 13C-labelled sodium octanoate breath test. Venous blood was drawn frequently for measurement of glucose, insulin, C-peptide, glucagon, GLP-1, triglycerides and NEFA. Results: GLP-1 administration lowered fasting and postprandial glycaemia (p<0.0001). Gastric emptying was delayed by GLP-1 compared with placebo (p<0.0001). During GLP-1 administration, insulin secretory responses were higher in the fasting state but lower after meal ingestion. After meal ingestion, triglyceride plasma levels increased by 0.33± 0.14 mmol/l in the placebo experiments (p<0.0001). In contrast, the postprandial increase in triglyceride levels was completely abolished by GLP-1 (change in triglycerides, -0.023± 0.045 mmol/l; p<0.05). During GLP-1 infusion, plasma concentrations of NEFA were suppressed by 39% in the fasting state (p<0.01) and by 31±5% after meal ingestion (p<0.01). Conclusions/interpretation: GLP-1 improves postprandial lipidaemia, presumably as a result of delayed gastric emptying and insulin-mediated inhibition of lipolysis. Thus, by lowering both glucose and lipid concentrations, GLP-1 administration may reduce the cardiovascular risk in patients with type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2006

14. Secretion of incretin hormones and the insulinotropic effect of gastric inhibitory polypeptide in women with a history of gestational diabetes.

Author

Meier, J. J., Gallwitz, B., Askenas, M., Vollmer, K., Deacon, C. F., Holst, J. J., Schmidt, W. E., and Nauck, M. A.

Subjects

SURROGATE mothers, DIABETES complications, CELL physiology, PEPTIDE hormones, DISEASES in women, INSULIN resistance, DISEASES

Abstract

Aims/hypothesis: The insulinotropic effect of gastric inhibitory polypeptide (GIP) is reduced in patients with type 2 diabetes and around 50% of their first-degree relatives under hyperglycaemic conditions. It is unknown whether this is a result of a specific defect in GIP action or of a general reduction in beta cell function. Moreover, impaired secretion of glucagon-like peptide 1 (GLP-1) has been described in patients with type 2 diabetes. Therefore, we studied the insulinotropic effect of GIP in women with previous gestational diabetes (pGDM) under euglycaemic fasting conditions and during a hyperglycaemic clamp experiment. The secretion of GIP and GLP-1 was assessed following oral glucose ingestion. Materials and methods: On separate occasions we performed an OGTT and administered an i.v. bolus of 20 pmol GIP/kg body weight in 20 women with pGDM and 20 control women. An additional hyperglycaemic clamp experiment (140 mg/dl [7.8 mmol/l] over 120 min) with i.v. infusion of GIP (2 pmol kg-1 min-1; 30–90 min) was performed in 14 women in each group. Capillary and venous blood samples were drawn for the measurement of glucose (glucose oxidase), insulin, C-peptide, GIP and GLP-1 (specific immunoassays). Indices of insulin sensitivity and beta cell function were calculated. Statistical analyses were carried out using repeated measures ANOVA. Results: Following oral glucose ingestion, plasma glucose, insulin and C-peptide concentrations increased to higher levels in the women with pGDM than in the control women (p«0.05). The women with pGDM were characterised by a higher degree of insulin resistance than the control women (p=0.007 for the Matsuda index), but showed no overt defects in glucose-stimulated insulin secretion (p=0.40 for the insulinogenic index following i.v. glucose). The secretion of GLP-1 and GIP was not different between the groups (p=0.87 and p=0.57, respectively). The insulin secretory response to GIP administration was similar in the two groups both after GIP bolus administration and during the hyperglycaemic clamp experiment (p=0.99 and p=0.88, respectively). A hyperbola-like relationship was found between the degree of insulin sensitivity (Matsuda index) and the insulin secretory response to GIP and i.v. glucose administration. Conclusions/interpretation: These results do not support the hypothesis of an early defect in GIP action as a risk factor for subsequent development of diabetes in women with previous gestational diabetes. The inverse relationship between insulin resistance and the insulin secretory response to glucose or GIP suggests that beta cell secretory function in response to different stimuli increases adaptively when insulin sensitivity is diminished. [ABSTRACT FROM AUTHOR]

Published

2005

15. Primärprävention beim Diabetes mellitus Typ 2.

Author

Gallwitz, B.

Abstract

Copyright of Der Internist is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2004

16. Gastric inhibitory polypeptide (GIP) dose-dependently stimulates glucagon secretion in healthy human subjects at euglycaemia J.J. Meier et al.: GIP and glucagon secretion.

Author

Meier, J. J., Gallwitz, B., Siepmann, N., Holst, J. J., Deacon, C. F., Schmidt, W. E., and Nauck, M. A.

Subjects

PANCREAS, GLUCAGON, GLUCOSE, PEPTIDE hormones, HYPERGLYCEMIA

Abstract

Aims/hypothesis. In the isolated perfused pancreas, gastric inhibitory polypeptide (GIP) has been shown to enhance glucagon secretion at basal glucose concentrations, but in healthy humans no glucagonotropic effect of GIP has yet been reported. Therefore, we studied the effect of GIP on glucagon secretion under normoglycaemic conditions. Methods. Ten healthy subjects (9 men, 1 woman; age 33±11; BMI 26.8±2.2 kg/m2) received three different doses of intravenous GIP (7, 20, and 60 pmol/kg body weight) and placebo. Venous blood samples were drawn over 30 min for glucagon and GIP concentrations (specific radioimmunoassays). In addition, 31 healthy subjects (16 men, 15 women; 42±11 years; BMI 24.4±2.7 kg/m2) were studied with 20 pmol GIP/kg. Statistics were done with RM-ANOVA and Duncan's post hoc tests. Results. Gastric inhibitory polypeptide dose-dependently stimulated glucagon secretion (p=0.019) with a maximal increment after 10 min. Incremental glucagon concentrations (Δ10–0 min) were 0.1±0.7, 1.4±0.5, 2.4±0.5, and 3.4±0.8 pmol/l (for placebo and for 7, 20, and 60 pmol GIP/kg, respectively; p=0.017). After the injection of 20 pmol GIP/kg b.w. in 31 healthy subjects, glucagon concentrations increased over the baseline from 7.5±0.5 to 9.3±0.7 pmol/l (p=0.0082). Conclusions/interpretation. Glucagon secretion is dose-dependently stimulated by GIP at basal glucose concentrations. The absence of a glucagonotropic GIP effect in previous studies could be due to the hyperglycaemic conditions used in these experiments. Our results underline differences between GIP and the glucagonostatic incretin GLP-1. [ABSTRACT FROM AUTHOR]

Published

2003

17. Insulinanaloga und neue Antidiabetika Perspektiven der Diabetestherapie.

Author

Gallwitz, B. and Schmidt, W.E.

Abstract

Copyright of Der Internist is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

1997

18. Impaired glucagon-like peptide-1-induced insulin secretion in carriers of transcription factor 7-like 2 (TCF7L2) gene polymorphisms.

Author

Schäfer, S., Tschritter, O., Machicao, F., Thamer, C., Stefan, N., Gallwitz, B., Holst, J., Dekker, J., t’Hart, L., Nijpels, G., Haeften, T., Häring, H., and Fritsche, A.

Published

2009

19. Impaired glucagon-like peptide-1-induced insulin secretion in carriers of transcription factor 7-like 2 ( TCF7L2) gene polymorphisms.

Author

Schäfer, S., Tschritter, O., Machicao, F., Thamer, C., Stefan, N., Gallwitz, B., Holst, J., Dekker, J., ’t Hart, L., Nijpels, G., Haeften, T., Häring, H., and Fritsche, A.

Published

2008