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Induction of oxidative stress causes functional alterations in mouse urothelium via a TRPM 8‐mediated mechanism: implications for aging
Author(s) -
Nocchi Linda,
Daly Donna M.,
Chapple Christopher,
Grundy David
Publication year - 2014
Publication title -
aging cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.103
H-Index - 140
eISSN - 1474-9726
pISSN - 1474-9718
DOI - 10.1111/acel.12208
Subject(s) - urothelium , oxidative stress , downregulation and upregulation , endocrinology , trpm8 , calcium in biology , overactive bladder , biology , calcium , medicine , transient receptor potential channel , receptor , urinary system , biochemistry , pathology , trpv1 , alternative medicine , gene
Summary The incidence of bladder conditions such as overactive bladder syndrome and its associated urinary incontinence is highly prevalent in the elderly. However, the mechanisms underlying these disorders are unclear. Studies suggest that the urothelium forms a ‘sensory network’ with the underlying innervation, alterations in which, could compromise bladder function. As the accumulation of reactive oxygen species can cause functional alterations with age, the aim of this study was to investigate whether oxidative stress alters urothelial sensory signalling and whether the mechanism underlying the effect of oxidative stress on the urothelium plays a role in aging. Five‐month‐old(young) and 24‐month‐old (aged) mice were used. H 2 O 2 , used to induce oxidative stress, resulted in an increase in bladder afferent nerve activity and urothelial intracellular calcium in preparations from young mice. These functional changes were concurrent with upregulation of TRPM 8 in the urothelium. Moreover, application of a TRPM 8 antagonist significantly attenuated the H 2 O 2 ‐induced calcium responses. Interestingly, an upregulation of TRPM 8 was also found in the urothelium from aged mice, where high oxidative stress levels were observed, together with a greater calcium response to the TRPM 8 agonist WS 12. Furthermore, these calcium responses were attenuated by pretreatment with the antioxidant N ‐acetyl‐cysteine. This study shows that oxidative stress affects urothelial function involving a TRPM 8‐mediated mechanism and these effects may have important implications for aging. These data provide an insight into the possible mechanisms by which oxidative stress causes physiological alterations in the bladder, which may also occur in other organs susceptible to aging.

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