Reduction of insulin signalling pathway IRS‐1/IRS‐2/AKT/mTOR and decrease of epithelial cell proliferation in the prostate of glucocorticoid‐treated rats

Costa, Maite M.; Violato, Natalia Moretti; Taboga, Sebastião Roberto; Góes, Rejane Maira; Bosqueiro, José Roberto

doi:10.1111/j.1365-2613.2012.00817.x

Cited by 21 publications

(14 citation statements)

References 49 publications

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“…IRs are present in most mammalian cells, and insulin-IR binding results in the activation of several phosphorylation-dephosphorylation cascades (11). Autophosphorylation of the intracellular β-subunit of IRs activates tyrosine kinase, which catalyzes multiple IR substrate (IRS) protein phosphorylation (12). Disruption in IRS protein phosphorylation or impaired PI3K recruitment from the cytosol, which results in PI3K inactivation, causes insulin resistance, followed by diabetes (13).…”

mentioning

confidence: 99%

White sweet potato ameliorates hyperglycemia and regenerates pancreatic islets in diabetic mice

Shih

Chen

Varga

et al. 2020

Food & Nutrition Research

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mentioning

confidence: 99%

White sweet potato ameliorates hyperglycemia and regenerates pancreatic islets in diabetic mice

Shih

Chen

Varga

et al. 2020

Food & Nutrition Research

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“…1, G-I; Fig. 2, G-I), we assessed UT temporal expression of the mammalian target of rapamycin (mTOR) and nerve growth factor (NGF), as these genes are reported to promote cell proliferation (22,35,72). As recent evidence supports a dependence of urothelial repair upon signal feedback between basal UT cells, the stromal cells that underlie them, and the sonic hedgehog (SHh) signaling pathway (69), we also examined temporal expression of SHh and its associated receptor patched 1 (Pct1) (40).…”

Section: Temporal Profile Of Ut Gene Expression In Dmmentioning

confidence: 99%

Impact of diabetes mellitus on bladder uroepithelial cells

Hanna-Mitchell

Ruiz

Daneshgari

et al. 2013

American Journal of Physiology-Regulatory, Integrative and Comp

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Diabetic bladder dysfunction (DBD), a prevalent complication of diabetes mellitus (DM), is characterized by a broad spectrum of symptoms including urinary urgency, frequency, and incontinence. As DBD is commonly diagnosed late, it is important to understand the chronic impact of DM on bladder tissues. While changes in bladder smooth muscle and innervation have been reported in diabetic patients, the impact of DM on the specialized epithelial lining of the urinary bladder, the urothelium (UT), is largely unknown. Quantitative polymerase chain reaction analysis and electron microscopy were used to evaluate UT gene expression and cell morphology 3, 9, and 20 wk following streptozotocin (STZ) induction of DM in female SpragueDawley rats compared with age-matched control tissue. Desquamation of superficial (umbrella) cells was noted at 9 wk DM, indicating a possible breach in barrier function. One causative factor may be metabolic burden due to chronic hyperglycemia, suggested by upregulation of the polyol pathway and glucose transport genes in DM UT. While superficial UT repopulation occurred by 20 wk DM, the phenotype was different, with significant upregulation of receptors associated with UT mechanosensation (transient receptor potential vanilloid subfamily member 1; TRPV1) and UT autocrine/paracrine signaling (acetylcholine receptors AChR-M2 and -M3, purinergic receptors P2X2 and P2X3). Compromised barrier function and alterations in UT mechanosensitivity and cell signaling could contribute to bladder instability, hyperactivity, and altered bladder sensation by modulating activity of afferent nerve endings, which appose the urothelium. Our results show that DM impacts urothelial homeostasis and may contribute to the underlying mechanisms of DBD. streptozotocin; urothelium; barrier; sensory; diabetic bladder dysfunction IN THE UNITED STATES alone it is estimated that approximately 19 million individuals, comprising both men and women, suffer from diabetes mellitus (DM) (13). DM is characterized by defects in the secretion of the hormone insulin by the pancreas and/or insulin signaling (53), which causes a dysregulation of cellular glucose uptake. Glucose is a large hydrophilic molecule that depends on specific glucose transporter (GLUT) proteins, present on the cell membrane, for cellular entry (12). From the GLUT family (13 cloned to date), GLUT4 is regulated by insulin and controls glucose uptake by skeletal muscle [which accounts for ϳ40% of total body mass (70)], cardiac muscle, and adipose tissue (75). Thus Type 1 and 2 diabetics are unable to efficiently transport glucose from the blood into these tissue groups (66) resulting in a state of hyperglycemia. Consequently, glucose inundates cells that express insulinindependent glucose transporters (such as GLUT1). Chronic elevation in cytosolic glucose leads to metabolic abnormalities such as osmotic and oxidative stress, thought to be factors that contribute to tissue injury and dysfunction associated with long-term DM (15, 61).The urinary bladder is one of th...

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“…Costa et al . () showed that the reduction in inhibition rate in animals treated with GCs leads to a reduction in plasma concentration of AKT and mTOR, proteins involved in the regulation of cell growth and development.…”

Section: Discussionmentioning

confidence: 99%

Corticosterone influences gerbil (Meriones unguiculatus) prostatic morphophysiology and alters its proliferation and apoptosis rates

Antoniassi

Fochi

Góes

et al. 2017

Int J Experimental Path

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Glucocorticoids (GCs) are hormones that are widely used in medicine; but although side effects are generally recognised, little is known about the precise mechanisms that is implicated in many of these side effects. Furthermore, GCs are highly correlated with stress and behaviour disorders. This study evaluated the effects of the glucocorticoid corticosterone on the ventral prostate of the Mongolian gerbil. Male gerbils (Meriones unguiculatus) (n = 5) received intraperitoneal injections of saline or corticosterone in doses of 0.5 mg/kg/day and 1.5 mg/kg/day for 5 days; while some of the animals were killed immediately after the treatment, the others were killed 5 days after the treatment period. The data show that corticosterone influences the structure and functionality of this organ. This hormone has anti-proliferative and anti-apoptotic properties in the prostate. In addition, the frequencies of the androgen (AR), oestrogen (ERα, ERβ) and glucocorticoid (GR) receptors changed. The frequencies of AR, GR and ERβ decreased in the Ct1/5 group; in the groups with rest period, the frequencies of GR increased and ERβ decreased in the epithelium. Changes in the proliferative index, apoptotic index and receptor activity may have contributed to the emergence of prostatic morphological alterations, such as the presence of cellular debris and inflammatory cells. Different doses of corticosterone had variable effects on the prostate, with a higher dose showing subtler effects and a lower dose showing more striking effects. The corticosterone effects on nuclear receptors were reverted or attenuated after a rest period, which was not observed for proliferation and apoptosis. In summary, we have demonstrated that corticosterone might influence the prostatic morphophysiology and that these changes may be linked in some way to the altered receptor distribution.

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Reduction of insulin signalling pathway IRS‐1/IRS‐2/AKT/mTOR and decrease of epithelial cell proliferation in the prostate of glucocorticoid‐treated rats

Cited by 21 publications

References 49 publications

White sweet potato ameliorates hyperglycemia and regenerates pancreatic islets in diabetic mice

White sweet potato ameliorates hyperglycemia and regenerates pancreatic islets in diabetic mice

Impact of diabetes mellitus on bladder uroepithelial cells

Corticosterone influences gerbil (Meriones unguiculatus) prostatic morphophysiology and alters its proliferation and apoptosis rates

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