Sodium channel mutation in irritable bowel syndrome: evidence for an ion channelopathy

Saito, Yuri; Strege, Peter R.; Tester, David J.; Locke, G. Richard; Talley, Nicholas J.; Bernard, Cheryl E.; Rae, James L.; Makielski, Jonathan C.; Ackerman, Michael J.; Farrugia, Gianrico

doi:10.1152/ajpgi.90571.2008

Cited by 117 publications

(128 citation statements)

References 30 publications

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“…Homozygous GNB3 825C carrier status is associated with unexplained upper abdominal symptoms in FD [35] and is linked to predominant EPStype FD in a Japanese population [36]. In IBS, a mutation identified in the Na v 1.5 sodium channel gene (SCN5A) has been identified in IBS [37], and may explain up to 2 % of IBS cases. Importantly, the sodium channel changes may be amenable to pharmacological intervention as suggested by a proof-of-principle study in one patient.…”

Section: Geneticsmentioning

confidence: 99%

Therapeutic strategies for functional dyspepsia and irritable bowel syndrome based on pathophysiology

2015

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Functional gastrointestinal disorders (FGIDs) are common and distressing. They are so named because a defined pathophysiology in terms of structural or biochemical pathways is lacking. Traditionally FGIDs have been conceptualized as brain-gut disorders, with subgroups of patients demonstrating visceral hypersensitivity and motility abnormalities as well as psychological distress. However, it is becoming apparent that there are certain structural or biochemical gut alterations among subsets with the common FGIDs, most notably functional dyspepsia (FD) and irritable bowel syndrome (IBS). For example, a sodium channel mutation has been identified in IBS that may account for 2 % of cases, and subtle intestinal inflammation has been observed in both IBS and FD. Other research has implicated early life events and stress, autoimmune disorders and atopy and infections, the gut microbiome and disordered mucosal immune activation in patients with IBS or FD. Understanding the origin of symptoms in FGIDs will allow therapy to be targeted at the pathophysiological changes, not at merely alleviating symptoms, and holds hope for eventual cure in some cases.For example, there are promising developments in manipulating the microbiome through diet, prebiotics and antibiotics in IBS, and testing and treating patients for Helicobacter pylori infection remains a mainstay of therapy in patients with dyspepsia and this infection. Locally acting drugs such as linaclotide have been an advance in treating the symptoms of constipation-predominant IBS, but do not alter the natural history of the disease. A role for a holistic approach to patients with FGIDs is warranted, as brain-togut and gut-to-brain pathways appear to be activated.

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Section: Geneticsmentioning

confidence: 99%

Therapeutic strategies for functional dyspepsia and irritable bowel syndrome based on pathophysiology

2015

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“…The Na v 1.5 voltage-gated sodium channel encoded by SCN5A is expressed in human jejunal epithelial cells and interstitial cells of Cajal (68). In a study of an IBS cohort, one patient with a family history of IBS exhibited a loss-of-function G298S missense mutation on a background of a common H558R polymorphism in SCN5A (69). The G298S mutation results in a reduction in the current density, slowing of the activation kinetics, and possibly reduced mechanosensitivity of the channel on H558R background (69).…”

Section: Visceral Painmentioning

confidence: 99%

“…In a study of an IBS cohort, one patient with a family history of IBS exhibited a loss-of-function G298S missense mutation on a background of a common H558R polymorphism in SCN5A (69). The G298S mutation results in a reduction in the current density, slowing of the activation kinetics, and possibly reduced mechanosensitivity of the channel on H558R background (69). Further studies are needed to establish an association of SCN5A channelopathies with IBS symptoms.…”

Section: Visceral Painmentioning

confidence: 99%

Pain as a channelopathy

Raouf¹,

Quick

Wood

2010

J. Clin. Invest.

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Mendelian heritable pain disorders have provided insights into human pain mechanisms and suggested new analgesic drug targets. Interestingly, many of the heritable monogenic pain disorders have been mapped to mutations in genes encoding ion channels. Studies in transgenic mice have also implicated many ion channels in damage sensing and pain modulation. It seems likely that aberrant peripheral or central ion channel activity underlies or initiates many pathological pain conditions. Understanding the mechanistic basis of ion channel malfunction in terms of trafficking, localization, biophysics, and consequences for neurotransmission is a potential route to new pain therapies.

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“…For example people with mutations in SCN5A have higher prevalence of Brugada syndrome and functional dyspepsia, 7 as well as irritable bowel syndrome (IBS). 8 Thus agents directly regulating ion channel activities either in ICC or in SMCs may affect the GI peristalsis. 9 For example, certain potassium channel blockers and compounds increasing Ca 2+ release or Ca 2+ sensitivity specifically acting on GI tract would be potentially effective therapeutic agents for GI dysmotility.…”

Section: Introductionmentioning

confidence: 99%

Targeting Ion Channels: An Important Therapeutic Implication in Gastrointestinal Dysmotility in Patients With Spinal Cord Injury

Radulovic

Anand

Korsten

et al. 2015

J Neurogastroenterol Motil

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Gastrointestinal (GI) dysmotility is a severe, and common complication in patients with spinal cord injury (SCI). Current therapeutic methods using acetylcholine analogs or laxative agents have unwanted side effects, besides often fail to have desired effect. Various ion channels such as ATP-sensitive potassium (KATP) channel, calcium ions (Ca 2+ )-activated potassium ions (K + ) channels, voltage-sensitive Ca 2+ channels and chloride ion (Cl − ) channels are abundantly expressed in GI tissues, and play an important role in regulating GI motility. The release of neurotransmitters from the enteric nerve terminal, innervating GI interstitial cells of Cajal (ICC), and smooth muscle cells (SMC), causes inactivation of K + and Cl − channels, increasing Ca 2+ influx into cytoplasm, resulting in membrane depolarization and smooth muscle contraction. Thus, agents directly regulating ion channels activity either in ICC or in SMC may affect GI peristalsis and would be potential therapeutic target for the treatment of GI dysmotility with SCI.

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Sodium channel mutation in irritable bowel syndrome: evidence for an ion channelopathy

Cited by 117 publications

References 30 publications

Therapeutic strategies for functional dyspepsia and irritable bowel syndrome based on pathophysiology

Therapeutic strategies for functional dyspepsia and irritable bowel syndrome based on pathophysiology

Pain as a channelopathy

Targeting Ion Channels: An Important Therapeutic Implication in Gastrointestinal Dysmotility in Patients With Spinal Cord Injury

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