Urethral dysfunction due to alloxan-induced diabetes. Urodynamic and morphological evaluation

Pegorare, Ana Beatriz Gomes de Souza; Gonçalves, Marco Antônio; Suaid, Carla Adelino; Rodrigues, Antônio Antunes; Tucci, Sílvio; Suaid, Haylton Jorge

doi:10.1590/s0102-86502014000700008

Cited by 3 publications

(6 citation statements)

References 22 publications

(29 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Acute surgically‐induced vesical denervation markedly increased BC and compliance in control and diabetic animals. A follow‐up study performed by the same group at 6 and 20 weeks after alloxan injection found no difference between control and diabetic animals for BC, voiding frequency or maximum pressure . Thus, except for the latter study, experiments in STZ‐injected mice and alloxan‐injected rats exhibited a similar cystometric profile as STZ‐injected rats.…”

Section: Exploration Of Links Between Hypertrophy and Bladder Dysfuncmentioning

confidence: 71%

“…On the other hand, the two studies on alloxan‐injected rabbits also reported a modest degree of hypertrophy only based on BW (127‐133% of control) . Another possible difference is that there was little further bladder enlargement beyond week 1 in the rat STZ model, whereas one study in alloxan‐injected rats reported a bladder wall thickness of 553 μm in control and 655 μm in diabetic animals after 6 weeks, which increased further to 899 μm after 20 weeks . Therefore, the alloxan model confirms the existence of bladder hypertrophy in T1DM models but despite a similar extent of blood glucose elevation appears to cause less hypertrophy than injection of STZ.…”

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 88%

“…While alloxan‐induced diabetes was also associated with bladder hypertrophy in rats and rabbits (Figure , Supplementary Table S1), there may be differences as compared to the STZ model. Thus, two studies with alloxan‐injected rats reported a BW of 187‐196% of control, whereas two later studies observed little hypertrophy (92‐118% of control) . Interpretation of these differences is complicated by the fact that the latter two studies have not reported on BW but on total bladder thickness.…”

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 99%

“…Thus, two studies with alloxan-injected rats reported a BW of 187-196% of control, 9,10 whereas two later studies observed little hypertrophy (92-118% of control). 11,12 Interpretation of these differences is complicated by the fact that the latter two studies have not reported on BW but on total bladder thickness. On the other hand, the two studies on alloxaninjected rabbits also reported a modest degree of hypertrophy only based on BW (127-133% of control).…”

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 99%

See 3 more Smart Citations

A systematic review of urinary bladder hypertrophy in experimental diabetes: Part 2. Comparison of animal models and functional consequences

Ellenbroek

İnan

Michel

2018

Neurourology and Urodynamics

View full text Add to dashboard Cite

show abstract

Section: Exploration Of Links Between Hypertrophy and Bladder Dysfuncmentioning

confidence: 71%

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 88%

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 99%

Section: Comparison Of Hypertrophy Among Models Of Type 1 Diabetesmentioning

confidence: 99%

See 2 more Smart Citations

A systematic review of urinary bladder hypertrophy in experimental diabetes: Part 2. Comparison of animal models and functional consequences

Ellenbroek

İnan

Michel

2018

Neurourology and Urodynamics

View full text Add to dashboard Cite

show abstract

“…Previous studies reported that the morphology of the urethra can also be altered in DM. For example, the urethras from 6 weeks and 20 weeks in alloxan-induced diabetic rats had greater values of total thickness than did the control rats whereas the urethra from 6- and 20-week DM rats had reduced thickness of the urothelium of the urethra [30]. In 6- and 20-week STZ-induced DM rats, the morphological images revealed that the striated muscle bundles in 20-week diabetic rats were atrophied compared with those of controls although no obvious changes were observed in the thickness of EUS of 6-week diabetic rats compared with controls (Fig.…”

Section: Preclinical Studymentioning

confidence: 99%

Time-Dependent Changes of Urethral Function in Diabetes Mellitus: A Review

Cao¹,

Gu²,

Gotoh³

et al. 2019

Int Neurourol J

View full text Add to dashboard Cite

This article reviewed the current knowledge on time-course manifestation of diabetic urethral dysfunction (DUD), and explored an early intervention target to prevent the contribution of DUD to the progression of diabetes-induced impairment of the lower urinary tract (LUT). In the literature search through PubMed, key words used included “diabetes mellitus,” “diabetic urethral dysfunction,” and “diabetic urethropathy.” Polyuria and hyperglycemia induced by diabetes mellitus (DM) can cause the time-dependent changes in functional and morphological manifestations of DUD. In the early stage, it promotes urethral dysfunction characterized by increased urethral pressure during micturition. However, the detrusor muscle of the bladder tries to compensate for inducing complete voiding by increasing the duration and amplitude of bladder contractions. As the disease progresses, it can induce an impairment of coordinated micturition due to dyssynergic activity of external urethra sphincter, leading to detrusor-sphincter dyssynergia. The impairment of relaxation mechanisms of urethral smooth muscles (USMs) may additionally be attributable to decreased responsiveness to nitric oxide, as well as increased USM responsiveness to α 1 -adrenergic receptor stimulation. In the late stage, diabetic neuropathy may play an important role in inducing LUT dysfunction, showing that the decompensation of the bladder and urethra, which can cause the decrease of voiding efficiency and the reduced thickness of the urothelium and the atrophy of striated muscle bundles, possibly leading to the vicious cycle of the LUT dysfunction. Further studies to increase our understandings of the functional and molecular mechanisms of DUD are warranted to explore potential targets for therapeutic intervention of DM-induced LUT dysfunction.

show abstract

Path of translational discovery of urological complications of obesity and diabetes

Daneshgari

Liu

Hanna-Mitchell

2017

American Journal of Physiology-Renal Physiology

View full text Add to dashboard Cite

Diabetes mellitus (DM) is a prevalent chronic disease. Type 1 DM (T1DM) is a metabolic disorder that is characterized by hyperglycemia in the context of absolute lack of insulin, whereas type 2 DM (T2DM) is due to insulin resistance-related relative insulin deficiency. In comparison with T1DM, T2DM is more complex. The natural history of T2DM in most patients typically involves a course of obesity to impaired glucose tolerance, to insulin resistance, to hyperinsulinemia, to hyperglycemia, and finally to insulin deficiency. Obesity is a risk factor of T2DM. Diabetes causes some serious microvascular and macrovascular complications, such as retinopathy, nephropathy, neuropathy, angiopathy and stroke. Urological complications of obesity and diabetes (UCOD) affect quality of life, but are not well investigated. The urological complications in T1DM and T2DM are different. In addition, obesity itself affects the lower urinary tract. The aim of this perspective is to review the available data, combined with the experience of our research teams, who have spent a good part of last decade on studies of association between DM and lower urinary tract symptoms (LUTS) with the aim of bringing more focus to the future scientific exploration of UCOD. We focus on the most commonly seen urological complications, urinary incontinence, bladder dysfunction, and LUTS, in obesity and diabetes. Knowledge of these associations will lead to a better understanding of the pathophysiology underlying UCOD and hopefully assist urologists in the clinical management of obese or diabetic patients with LUTS.

show abstract

Urethral dysfunction due to alloxan-induced diabetes. Urodynamic and morphological evaluation

Cited by 3 publications

References 22 publications

A systematic review of urinary bladder hypertrophy in experimental diabetes: Part 2. Comparison of animal models and functional consequences

A systematic review of urinary bladder hypertrophy in experimental diabetes: Part 2. Comparison of animal models and functional consequences

Time-Dependent Changes of Urethral Function in Diabetes Mellitus: A Review

Path of translational discovery of urological complications of obesity and diabetes

Contact Info

Product

Resources

About