Highly Variable Gastric Emptying in Patients With Insulin Dependent Diabetes Mellitus

Nowak, T. V., Johnson, C. P., Kalbfleisch, J. H., Roza, A. M., Wood, C. M., Weisbruch, J. P., Soergel, K. H.

01 January 1995

Some diabetic patients - particularly those with nausea and vomiting - frequently have evidence of delayed gastric emptying while other diabetic patients may in fact exhibit accelerated gastric emptying. Whether the presence or absence of symptoms of upper gastrointestinal dysfunction correlated with objective measures of gastric emptying in insulin dependent diabetic subjects was investigated. Twenty one insulin dependent diabetic patients underwent a solid phase gastric emptying scintiscan using in vivo labelled chicken patients had symptoms Thirteen patients had symptoms suggestive of gastrointestinal dysfunction (nausea, vomiting, early satiety, or constipation), while eight patients had no gastrointestinal symptoms. Eleven patients had orthostatic hypotension. All patients had been diabetic since childhood or adolescence. As a group, the diabetic patients showed a half time (T50) of gastric emptying (mean (SD) 150.0 min (163.7) that was not significantly different from that of 12 healthy control subjects (148.1 min (62.4)). Those diabetic patients without gastrointestinal symptoms and without orthostatic hypotension, however, showed a gastric emptying half time (70.1 min (41.6)) that was significantly faster than that of the control subjects. Conversely, those diabetic patients with nausea, vomiting, and early satiety (or early satiety alone) showed T50 values that were significantly greater than those of the diabetic patients without these symptoms. No correlation was found between the T50 value and the duration of diabetes, the fasting blood glucose at the time of study, or the respiratory variation in heart rate (E:I ratio). These observations indicate that highly variable rates of gastric emptying occur in insulin dependent diabetic patients, and that accelerated gastric emptying may occur in diabetic patients who have no symptoms of gastrointestinal dysfunction.

autonomic neuropathy

gastric emptying

Assessment of cardiac autonomic neuropathy (CAN) in Type I diabetic mice

Yang, Bufan

06 November 2011

"Diabetic cardiovascular autonomic neuropathy (DCAN) is common in patients with diabetes mellitus, and causes abnormalities in heart rate control as well as central and peripheral nervous system dynamics. A good understanding of DCAN is not established yet. An effective way to detect diabetes mellitus at an early stage is still undiscovered, which method is highly desired by researchers and patients. One reason why the pathogenesis of DCAN is unclear is that non- invasive assessment of DCAN in humans and animals has been problematic. The non-stationary and non- linear natures of the interested physiological signals have placed great limitation on traditionally algorithms. To overcome this limitation, this work proposes a series of time- varying, nonlinear and non-invasive methods to assess cardiac autonomic dysregulation from ECG and PPG records. Including a non-stationary method called PDM, which is based on principal dynamic mode (PDM) analysis of heart rate variability (HRV), nonstationary power spectral density called TVOPS-VFCDM and also standard spectrum analysis method of HRV. We are also able to study and analyze a series of long term and short term ECG and PPG data. In a pilot study, ECG was measured via telemetry in conscious 4 month old C57/Bl6 controls and in Akita mice, a model of insulin- dependent type I diabetes, while PPG was measured via tail pulse oximetry system from 2 month old to 4 month old. The results indicate significant cardiac autonomic impairment in the diabetic mice in comparison to the controls at 4 month old and such impairment start to present at 3 month old. Further, both immunohistochemistry and Western blot analyses show a reduction in nerve density in Akita mice as compared to the control mice, thus, corroborating our data analysis records."

HRV

PDM

akita mice

cardiac autonomic neuropathy

Clinical and Molecular Biological Studies in Hirschsprung's Disease

Croaker, Geoffrey David Hain

January 2002

HSCR has been felt to be a polygeneic disease on the basis of an incompletely penetrant sex modified transmission, which may be either autosomal dominant or recessive in different kindred. During the 1990's several of the genes involved in this transmission have come to light. Other genes remain to be discovered.

Clinical and Molecular Biological Studies in Hirschsprung's Disease

Croaker, Geoffrey David Hain

January 2002

HSCR has been felt to be a polygeneic disease on the basis of an incompletely penetrant sex modified transmission, which may be either autosomal dominant or recessive in different kindred. During the 1990's several of the genes involved in this transmission have come to light. Other genes remain to be discovered.

Postprandial hypotension: hemodynamic differences between multiple system atrophy and peripheral autonomic neuropathy

Takahashi, A, Hakusui, S, Sakurai, N, Kanaoke, Y, Hasegawa, Y, Koike, Y, Watanabe, H, Hirayama, M

04 1900

名古屋大学博士学位論文 学位の種類 : 博士(医学)(論文) 学位授与年月日:平成5年1月28日 平山正昭氏の博士論文として提出された

Autonomic neuropathy

Multiple system atrophy

Hemodynamics

Cardiac output

Postprandial hypotension

Effect of Cyclooxygenase (COX)-2 Activation on Diabetic Neuropathy

Kellogg, Aaron

18 June 2008

No description available.

Molecular Biology

diabetes

cyclooxygenase-2

peripheral neuropathy

cardiac autonomic neuropathy

Avaliação do efeito da administração de piridostigmina sobre a variabilidade da frequência cardíaca em pacientes portadores de diabetes mellitus tipo 2 com neuropatia autonômica cardiovascular

Harthmann, Ângela d'Avila

January 2010

Objetivos/Hipótese: A Piridostigmina bloqueia a acetilcolinesterase, promove estimulação colinérgica e aumenta a variabilidade da freqüência cardíaca (VFC) em indivíduos saudáveis e com insuficiência cardíaca. Os efeitos sobre a modulação autonômica no diabetes mellitus tipo 2 (DM2) são desconhecidos. Nós testamos a hipótese de que a administração de piridostigmina aumenta a VFC em pacientes com DM2 e neuropatia autonômica cardiovascular (NAC). Métodos: Estudamos 34 pacientes com DM2 e NAC com idade entre 30 e 70 anos. Dezessete receberam 30 mg de piridostigmina via oral, de 8/8h por 24h (PI) e 17 receberam placebo (PL). A VFC foi avaliada pela média (RRMed) e desvio padrão dos intervalos RR (SDNN), pela raiz quadrada da média das diferenças sucessivas entre intervalos RR (RMSSD) e pelos índices do Mapa de Retorno Tridimensional P1, P2, P3 e MN. Resultados: Não houve diferenças significativas entre os grupos PI e PL quanto às características clínicas basais e à VFC sob efeito de piridostigmina e PL (RRMed - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusão: A piridostigmina não modifica a VFC em pacientes com DM2 e NAC. / Aims/Hypothesis: Pyridostigmine blocks acetylcholinesterase, promotes cholinergic stimulation and increases heart rate variability (HRV) in healthy individuals and with cardiac heart failure. The effects on the autonomic modulation in diabetes mellitus type 2 (DM2) are unknown. We have tested the hypothesis that the administration of pyridostigmine increases HRV in DM2 and CAN patients (CAN). Methods: We have studied 34 DM2 and CAN patients aged between 30 and 70 years old. Seventeen received 30mg of pyridostigmine via oral administration, every 8 hours during 24 hours (PY) and 17 received placebo (PL). HRV was assessed by the mean of all normal R-R intervals RR (mean RR) and the standard deviation of all normal R-R intervals (SDNN), by the root-mean-square of successive differences (RMSSD) and by the three-dimensional return map indices P1, P2, P3 and MN. Results: There were no significant differences between the PY and PL groups as to the baseline clinical characteristics and to HRV under the effect of pyridostigmine and PL (mean RR - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusion: Pyridostigmine does not modify HRV in DM2 and CAN patients.

Diabetes mellitus tipo 2

Neuropatias diabéticas

Frequência cardíaca

Diabetes mellitus

Autonomic neuropathy

Heart rate variability

Pyridostigmine

Avaliação do efeito da administração de piridostigmina sobre a variabilidade da frequência cardíaca em pacientes portadores de diabetes mellitus tipo 2 com neuropatia autonômica cardiovascular

Harthmann, Ângela d'Avila

January 2010

Objetivos/Hipótese: A Piridostigmina bloqueia a acetilcolinesterase, promove estimulação colinérgica e aumenta a variabilidade da freqüência cardíaca (VFC) em indivíduos saudáveis e com insuficiência cardíaca. Os efeitos sobre a modulação autonômica no diabetes mellitus tipo 2 (DM2) são desconhecidos. Nós testamos a hipótese de que a administração de piridostigmina aumenta a VFC em pacientes com DM2 e neuropatia autonômica cardiovascular (NAC). Métodos: Estudamos 34 pacientes com DM2 e NAC com idade entre 30 e 70 anos. Dezessete receberam 30 mg de piridostigmina via oral, de 8/8h por 24h (PI) e 17 receberam placebo (PL). A VFC foi avaliada pela média (RRMed) e desvio padrão dos intervalos RR (SDNN), pela raiz quadrada da média das diferenças sucessivas entre intervalos RR (RMSSD) e pelos índices do Mapa de Retorno Tridimensional P1, P2, P3 e MN. Resultados: Não houve diferenças significativas entre os grupos PI e PL quanto às características clínicas basais e à VFC sob efeito de piridostigmina e PL (RRMed - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusão: A piridostigmina não modifica a VFC em pacientes com DM2 e NAC. / Aims/Hypothesis: Pyridostigmine blocks acetylcholinesterase, promotes cholinergic stimulation and increases heart rate variability (HRV) in healthy individuals and with cardiac heart failure. The effects on the autonomic modulation in diabetes mellitus type 2 (DM2) are unknown. We have tested the hypothesis that the administration of pyridostigmine increases HRV in DM2 and CAN patients (CAN). Methods: We have studied 34 DM2 and CAN patients aged between 30 and 70 years old. Seventeen received 30mg of pyridostigmine via oral administration, every 8 hours during 24 hours (PY) and 17 received placebo (PL). HRV was assessed by the mean of all normal R-R intervals RR (mean RR) and the standard deviation of all normal R-R intervals (SDNN), by the root-mean-square of successive differences (RMSSD) and by the three-dimensional return map indices P1, P2, P3 and MN. Results: There were no significant differences between the PY and PL groups as to the baseline clinical characteristics and to HRV under the effect of pyridostigmine and PL (mean RR - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusion: Pyridostigmine does not modify HRV in DM2 and CAN patients.

Diabetes mellitus tipo 2

Neuropatias diabéticas

Frequência cardíaca

Diabetes mellitus

Autonomic neuropathy

Heart rate variability

Pyridostigmine

Avaliação do efeito da administração de piridostigmina sobre a variabilidade da frequência cardíaca em pacientes portadores de diabetes mellitus tipo 2 com neuropatia autonômica cardiovascular

Harthmann, Ângela d'Avila

January 2010

Objetivos/Hipótese: A Piridostigmina bloqueia a acetilcolinesterase, promove estimulação colinérgica e aumenta a variabilidade da freqüência cardíaca (VFC) em indivíduos saudáveis e com insuficiência cardíaca. Os efeitos sobre a modulação autonômica no diabetes mellitus tipo 2 (DM2) são desconhecidos. Nós testamos a hipótese de que a administração de piridostigmina aumenta a VFC em pacientes com DM2 e neuropatia autonômica cardiovascular (NAC). Métodos: Estudamos 34 pacientes com DM2 e NAC com idade entre 30 e 70 anos. Dezessete receberam 30 mg de piridostigmina via oral, de 8/8h por 24h (PI) e 17 receberam placebo (PL). A VFC foi avaliada pela média (RRMed) e desvio padrão dos intervalos RR (SDNN), pela raiz quadrada da média das diferenças sucessivas entre intervalos RR (RMSSD) e pelos índices do Mapa de Retorno Tridimensional P1, P2, P3 e MN. Resultados: Não houve diferenças significativas entre os grupos PI e PL quanto às características clínicas basais e à VFC sob efeito de piridostigmina e PL (RRMed - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusão: A piridostigmina não modifica a VFC em pacientes com DM2 e NAC. / Aims/Hypothesis: Pyridostigmine blocks acetylcholinesterase, promotes cholinergic stimulation and increases heart rate variability (HRV) in healthy individuals and with cardiac heart failure. The effects on the autonomic modulation in diabetes mellitus type 2 (DM2) are unknown. We have tested the hypothesis that the administration of pyridostigmine increases HRV in DM2 and CAN patients (CAN). Methods: We have studied 34 DM2 and CAN patients aged between 30 and 70 years old. Seventeen received 30mg of pyridostigmine via oral administration, every 8 hours during 24 hours (PY) and 17 received placebo (PL). HRV was assessed by the mean of all normal R-R intervals RR (mean RR) and the standard deviation of all normal R-R intervals (SDNN), by the root-mean-square of successive differences (RMSSD) and by the three-dimensional return map indices P1, P2, P3 and MN. Results: There were no significant differences between the PY and PL groups as to the baseline clinical characteristics and to HRV under the effect of pyridostigmine and PL (mean RR - 748 ± 99 vs 733 ± 111ms; SDNN - 107 ± 26 vs 108 ± 36ms; RRMSD - 20,7 ± 12,7 vs 20,3 ± 10ms; P1 - 63 ± 11 vs 69 ± 14; P2 - 66 ±13 vs 63 ± 15; P3 - 86 ± 34 vs 80 ± 24 e MN - 392 ± 241 vs 369 ± 185). Conclusion: Pyridostigmine does not modify HRV in DM2 and CAN patients.

Diabetes mellitus tipo 2

Neuropatias diabéticas

Frequência cardíaca

Diabetes mellitus

Autonomic neuropathy

Heart rate variability

Pyridostigmine

Correlates of autonomic nervous system function in a general population with special reference to HbA₁c: The Nagahama study / 一般住民における自律神経機能と特にHbA₁cとの関連：ながはまスタディ

Takahashi, Naomi

25 January 2021

京都大学 / 0048 / 新制・課程博士 / 博士(社会健康医学) / 甲第22888号 / 社医博第112号 / 新制||社医||11(附属図書館) / 京都大学大学院医学研究科社会健康医学系専攻 / (主査)教授 川上 浩司, 教授 今中 雄一, 教授 稲垣 暢也 / 学位規則第4条第1項該当 / Doctor of Public Health / Kyoto University / DFAM

Autonomic nervous system

HbA1c

Diabetes mellitus

Diabetic autonomic neuropathy

Heart rate variability

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