Inhalation anaesthetic isoflurane inhibits the muscarinic cation current and carbachol-induced gastrointestinal smooth muscle contractions

Dryn, Dariia O.; Luo, Jialie; Melnyk, Mariia I.; Zholos, Alexander; Hu, Hongzhen

doi:10.1016/j.ejphar.2017.11.044

Cited by 17 publications

(18 citation statements)

References 34 publications

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“…Overall, ketamine induced inhibition of mI CAT is highly reminiscent of the effects of isoflurane (Dryn et al, 2018). To our knowledge, our experiments provide first indication that G-proteins can be inhibited by ketamine, but obviously much further work is required to clarify the underlying mechanism.…”

Section: Discussionmentioning

confidence: 72%

“…The ileum longitudinal smooth muscle (SM) layer was rapidly removed by carefully peeling the SM in the longitudinal direction and placed into a normal physiological salt solution (PSS) containing (in mM): NaCl 120, glucose 12, HEPES 10, KCl 6, CaCl 2 2.5, MgCl 2 1.2, pH 7.4 (adjusted with NaOH). SM cells were isolated by enzymatic digestion using (in mg/ml) 1 collagenase type 1A, 1 soybean trypsin inhibitor II-S, 1.5 bovine serum albumin in divalent cation-free PSS following tissue incubated for 18 min at 36.5°C, as described in more detail elsewhere (Dryn et al, 2018).…”

Section: Cells Isolationmentioning

confidence: 99%

“…SM preparations and cells were randomly assigned to various tests and data analysis was performed independently in a semiblinded manner whenever possible (it should be noted that the inhibitory effects of ketamine were fairly obvious to the operator even without data analysis). Group size was determined based on our previous extensive experience studying mI CAT , and in particular on our recent similar study of mI CAT inhibition produced by isoflurane (Dryn et al, 2018). Current amplitudes were normalized by cell capacitance to account for variations in cell size.…”

Section: Measurements and Statistical Analysismentioning

confidence: 99%

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Suppression of mICAT in Mouse Small Intestinal Myocytes by General Anaesthetic Ketamine and its Recovery by TRPC4 Agonist (-)-englerin A

et al. 2020

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A better understanding of the negative impact of general anesthetics on gastrointestinal motility requires thorough knowledge of their molecular targets. In this respect the muscarinic cationic current (mICAT carried mainly via TRPC4 channels) that initiates cholinergic excitation-contraction coupling in the gut is of special interest. Here we aimed to characterize the effects of one of the most commonly used “dissociative anesthetics”, ketamine, on mICAT. Patch-clamp and tensiometry techniques were used to investigate the mechanisms of the inhibitory effects of ketamine on mICAT in single mouse ileal myocytes, as well as on intestinal motility. Ketamine (100 µM) strongly inhibited both carbachol- and GTPγS-induced mICAT. The inhibition was slow (time constant of about 1 min) and practically irreversible. It was associated with altered voltage dependence and kinetics of mICAT. In functional tests, ketamine suppressed both spontaneous and carbachol-induced contractions of small intestine. Importantly, inhibited by ketamine mICAT could be restored by direct TRPC4 agonist (-)-englerin A. We identified mICAT as a novel target for ketamine. Signal transduction leading to TRPC4 channel opening is disrupted by ketamine mainly downstream of muscarinic receptor activation, but does not involve TRPC4 per se. Direct TRPC4 agonists may be used for the correction of gastrointestinal disorders provoked by general anesthesia.

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Section: Discussionmentioning

confidence: 72%

Section: Cells Isolationmentioning

confidence: 99%

Section: Measurements and Statistical Analysismentioning

confidence: 99%

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Suppression of mICAT in Mouse Small Intestinal Myocytes by General Anaesthetic Ketamine and its Recovery by TRPC4 Agonist (-)-englerin A

et al. 2020

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“…Tsvilovskyy et al concluded that TRPC4 and TRPC6 channel activation are critical for stimulating the muscarinic cation current (mICAT) in intestinal smooth muscle [ 255 , 256 ], indicating that the mICAT may consist of TRPC4 and TRPC6 and that their activation may be important for accelerating intestinal motility. It has been reported that the inhibitory effect of anesthetic agents, such as isoflurane, decreasing gastrointestinal tract motility is mediated by inhibiting the G-protein signaling that is important for stimulation of mICAT formed by TRPC4 and TRPC6 channels [ 257 ]. However, the reports on the function of TRPCs in the gastrointestinal tract are scarce and new investigations are needed to better understand their contribution to regulating gut function.…”

Section: Physiological and Pathological Functions Of Trpcs Revealementioning

confidence: 99%

Transient Receptor Potential Canonical (TRPC) Channels: Then and Now

Chen

Sooch

Demaree

et al. 2020

Cells

101

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Twenty-five years ago, the first mammalian Transient Receptor Potential Canonical (TRPC) channel was cloned, opening the vast horizon of the TRPC field. Today, we know that there are seven TRPC channels (TRPC1–7). TRPCs exhibit the highest protein sequence similarity to the Drosophila melanogaster TRP channels. Similar to Drosophila TRPs, TRPCs are localized to the plasma membrane and are activated in a G-protein-coupled receptor-phospholipase C-dependent manner. TRPCs may also be stimulated in a store-operated manner, via receptor tyrosine kinases, or by lysophospholipids, hypoosmotic solutions, and mechanical stimuli. Activated TRPCs allow the influx of Ca2+ and monovalent alkali cations into the cytosol of cells, leading to cell depolarization and rising intracellular Ca2+ concentration. TRPCs are involved in the continually growing number of cell functions. Furthermore, mutations in the TRPC6 gene are associated with hereditary diseases, such as focal segmental glomerulosclerosis. The most important recent breakthrough in TRPC research was the solving of cryo-EM structures of TRPC3, TRPC4, TRPC5, and TRPC6. These structural data shed light on the molecular mechanisms underlying TRPCs’ functional properties and propelled the development of new modulators of the channels. This review provides a historical overview of the major advances in the TRPC field focusing on the role of gene knockouts and pharmacological tools.

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“…Activated receptors result in the contraction of gastrointestinal smooth muscles via Ca 2+ influx. There are reports that the activated muscarinic receptor opens non-selective cation channels which depolarizes the membrane in guinea-pig jejunal smooth muscles [ 33 ], that TRPC4 and TRPC6 are involved in visceral smooth muscle contractility induced by ACh [ 10 , 15 ], and that TRPC3/C6/C7 are involved in Ca 2+ currents mediated by muscarinic receptor [ 19 ]. In the stressed ileum, in contrast, the second half of the EFS-induced contraction was suppressed by 80% under atropine-treated conditions.…”

Section: Discussionmentioning

confidence: 99%

Gastrointestinal motility modulation by stress is associated with reduced smooth muscle contraction through specific transient receptor potential channel

Azuma

Suzuki

Nishiyama

et al. 2021

The Journal of Veterinary Medical Science

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Excessive stress response causes disability in social life. There are many diseases caused by stress, such as gastrointestinal motility disorders, depression, eating disorders, and cardiovascular diseases. Transient receptor potential (TRP) channels underlie nonselective cation currents and are downstream effectors of G protein-coupled receptors. Ca 2+ influx is important for smooth muscle contraction, which is responsible for gastrointestinal motility. Little is known about the possible involvement of TRP channels in the gastrointestinal motility disorders due to stress. The purpose of this study was to measure the changes in gastrointestinal motility caused by stress and to elucidate the mechanism of these changes. The stress model used the water immersion restraint stress. Gastrointestinal motility, especially the ileum, was recorded responses to electric field stimulation (EFS) by isometric transducer. EFS-induced contraction was significantly reduced in the ileum of stressed mouse. Even under the conditions treated with atropine, EFS-induced contraction was significantly reduced in the ileum of stressed mouse. In addition, carbachol-induced, neurokinin A-induced, and substance P-induced contractions were all significantly reduced in the ileum of stressed mouse. Furthermore, the expression of TRPC3 was decreased in the ileum of stressed mouse. These results suggest that the gastrointestinal motility disorders due to stress is associated with specific non-selective cation channel.

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Inhalation anaesthetic isoflurane inhibits the muscarinic cation current and carbachol-induced gastrointestinal smooth muscle contractions

Cited by 17 publications

References 34 publications

Suppression of mICAT in Mouse Small Intestinal Myocytes by General Anaesthetic Ketamine and its Recovery by TRPC4 Agonist (-)-englerin A

Suppression of mICAT in Mouse Small Intestinal Myocytes by General Anaesthetic Ketamine and its Recovery by TRPC4 Agonist (-)-englerin A

Transient Receptor Potential Canonical (TRPC) Channels: Then and Now

Gastrointestinal motility modulation by stress is associated with reduced smooth muscle contraction through specific transient receptor potential channel

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