Effects of a cannabinoid receptor agonist on colonic motor and sensory functions in humans: a randomized, placebo-controlled study

Esfandyari, Tuba; Camilleri, Michael; Busciglio, Irene; Burton, Duane D.; Baxter, Kari; Zinsmeister, Alan R.

doi:10.1152/ajpgi.00565.2006

Cited by 99 publications

(108 citation statements)

References 32 publications

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“…Nevertheless, there is not a clear correlation between compliance and pain perception (Käll et al, 2007;Lindström et al, 2008;Ravnefjord et al, 2008). Experimental data in humans showed that the nonselective cannabinoid dronabinol reduced colonic tone and increased compliance while increasing sensation ratings to distension, probably through the central modulation of perception (Esfandyari et al, 2007). In the present experiments, WIN55,212-2, at analgesic doses, did not modify the pressure-volume relationship during distension indicating a lack of effect modulating colonic compliance.…”

Section: Discussioncontrasting

confidence: 67%

“…Recent studies in several species, including humans, support a role for endocannabinoids modulating visceral pain (Jaggar et al, 1998;Farquhar-Smith et al, 2002;Sanson et al, 2006;Esfandyari et (2006) implicated CB 1/2 Rs in the modulation of basal viscerosensitivity in rats. However, according to the present results, CB 1 Rs account for the full analgesic effects of cannabinoids on basal CRD-associated pain responses.…”

Section: Discussionmentioning

confidence: 99%

“…According to these studies, both CB 1 Rs and CB 2 Rs elicited analgesic responses under basal conditions (Sanson et al, 2006) and during states of inflammation-induced hyperalgesia (Sanson et al, 2006;Kikuchi et al, 2008). Interestingly, the only data available in humans showed that the CB 1 /CB 2 nonselective agonist, dronabinol, relaxed the colon but increased sensation ratings to distension in healthy volunteers (Esfandyari et al, 2007). This was interpreted as an interaction between the colonic motor effects and the central action of cannabinoids modulating perception (increasing awareness).…”

Section: Introductionmentioning

confidence: 99%

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CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

Brusberg¹,

Arvidsson²,

Kang³

et al. 2009

J. Neurosci.

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Activation of cannabinoid receptors (CB 1 , CB 2 and GPR 55 ) produces analgesic effects in several experimental pain models, including visceral pain arising from the gastrointestinal tract. We assessed the role of CB 1 , CB 2 , and GPR 55 receptors and the endogenous cannabinoid system on basal pain responses and acute mechanical hyperalgesia during colorectal distension (CRD) in rodents. The effects of cannabinoid receptor agonists and antagonists on pain-related responses to CRD were assessed in rats and in wild-type and CB 1 receptor knock-out mice. The dual CB 1/2 agonist, WIN55,212-2, and the peripherally acting CB 1 -selective agonist, SAB-378, inhibited pain-related responses to repetitive noxious CRD (80 mmHg) in a dose-related manner in rats. The analgesic effects of WIN55,212-2 and SAB-378 were blocked by the selective CB 1 antagonist SR141716, but were not affected by the selective CB 2 antagonist SR144528. SR141716, per se, increased the responses to repetitive noxious CRD, indicative of hyperalgesia, and induced pain-related responses during non-noxious CRD (20 mmHg), indicative of allodynia. The cannabinoid receptor agonists anandamide, virodhamine and O-1602 had no effect. At analgesic doses, WIN55,212-2 did not affect colonic compliance. In accordance to the rat data, WIN55,212-2 produced analgesia, whereas SR141716 induced hyperalgesia, during noxious CRD (55 mmHg) in wild-type but not in CB 1 -knock-out mice. These data indicate that peripheral CB 1 receptors mediate the analgesic effects of cannabinoids on visceral pain from the gastrointestinal tract. The allodynic and hyperalgesic responses induced by SR141716 suggest the existence of an endogenous cannabinoid tone and the activation of CB 1 receptors during noxious CRD.

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Section: Discussioncontrasting

confidence: 67%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

Brusberg¹,

Arvidsson²,

Kang³

et al. 2009

J. Neurosci.

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“…45,46 VİSERAL DUYARLILIK CB'lerin viseral ağrı üzerine etkili olduğu birçok hayvan çalışmasında gösterilmiştir. CB1 ve CB2 reseptör agonistlerinin hem kolorektal distansiyon ile oluştu-rulmuş ağrı modelinde hem de inflamatuar uyaran ile oluşturulmuş viseral ağrı modelinde etkili olduğu gös-terilmiştir.…”

Section: Gastroi̇ntesti̇nal Moti̇li̇te üZeri̇ne Etki̇leri̇unclassified

“…46 Ancak bu hasta grubunda uyuşukluk, baş dönmesi ve sersemlik gibi yan etkilerin olması nedeni ile daha düşük dozlarda (2,5 ve 5 mg) ilacın kullanıl-dığı bir çalışmada, hastalarda tedavide fayda göz-lenmemiştir. 55 CB'lerin güçlü antiinflamatuar ve immünmo-dülator etkileri olması nedeni ile inflamatuar ve ağrı ile seyreden inflamatuar barsak hastalıkları (İBH)'nda etkin olabileceği düşünülmüştür.…”

Section: Kannabi̇noi̇dler Ve İnsan çAlişmalariunclassified

Endogenous Cannabinoid System and Its Role in Gastrointestinal Tract: Review

Sakin¹,

Doğrul²,

Kekilli³

et al. 2015

Turkiye Klinikleri J Gastroenterohepatol

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Ö ÖZ ZE ET T Esrar (Cannabis sativa) yüzyıllardır inflamatuar barsak hastalıkları, gastroenterit, anoreksi, motilite bozuklukları, diyare, diyabetik gastroparezi, kusma ve abdominal ağrı gibi sağlık problemlerinin tedavisinde kullanılmaktadır. Ancak kannabis ve sentetik kannabinoidlerin ciddi nö-ropsikiyatrik yan etkileri nedeni ile modern tıpta kullanımı sınırlıdır. Etken maddesi olan delta-9 tetrahidrokannabinol ve bu maddenin üzerinden etkili olduğu CB1 ve CB2 reseptörlerinin tanımlanmasından sonra endojen kannabinoid sistemin in vivo birçok etkisi olduğu gözlenmiştir. Bütün kannabinoid agonistler CB1 ve CB2 reseptörler üzerinden etki göstermektedir. İnsan vücu-dunda bu reseptörler üzerinden etki ederek memeli dokusunda endojen kannabinoid reseptörleri aktive eden anandamid ve 2-araşidonil gliserol gibi endokannabinoidler saptanmıştır. Lipid yapıdaki bu maddeler üretildikten hemen sonra hücrelerden salınırlar ve CB1 ve CB2 reseptörleri aktive ederek biyolojik yanıt oluştururlar. Kannabinoid sistemi oluşturan kannabinoid reseptörler, endokannabinoidler ve endokannabinoid sentez ve inaktivasyonunda rol oynayan enzimler özellikle enterik sinir sisteminde başta olmak üzere tüm gastrointestinal kanalda yaygın olarak saptanmıştır. Yapılan çalışmalarla kannabinoid sistemin gastrointestinal kanalda birçok farmakolojik etkisi olduğu gösterilmiştir. Kannabinoid sistem modülasyonunun hastalık fizyopatolojisi ve tedavisinde yer alabileceği hayvan çalışmalarında gösterilmiştir. Son yıllarda hayvan deneylerinde gözlenen bu faydalı etkileri nedeni ile, kannabinoid sistem üzerinde etkili ilaçlar insanlarda bazı hastalıkların tedavisinde denenmiştir ve hâlen denenmektedir. Bu çalışmada, endojen kannabinoid sistemin patofizyolojisini ve endojen kannabinoid sistem ile onun düzenleyicilerinin gastrointestinal kanalda oluşturduğu etkileri tanımlamak amaçlanmıştır.A An na ah ht ta ar r K Ke el li im me el le er r: : Kannabis; gastrointestinal hastalıklar; gastrointestinal kanal A AB BS ST TR RA AC CT T Cannabis sativa has been used to treat gastrointestinal diseases such as inflammatory bowel diseases, anorexia, motility disorders, diarrhea, gastroparesis, vomiting and abdominal pain for centuries. However, the use of cannabis is limited in modern medicine due to its neuropsychiatric side effects. After isolation of active ingredient delta-9 tetrahydrocannabinol and CB1 and CB2 receptors, the cannabinoid system and its various effects were determined. All of the cannabinoid agonists are acting on CB1 and CB2 receptors. Additionally, endocannabinoids such as anandamide and 2-arachyldonyl glycerol were defined in human body which activate endogenous cannabinoid receptors on mammalian tissue. Cannabinoid receptors, endocannabinoids and the enzymes which modulate synthesis and degradation of endocannabinoids were detected throughout the gastrointestinal canal, especially enteric nervous system. Many pharmacologic effects of cannabinoid system on gastrointestinal tract have been observed. At last decade, modulation of cannabinoid syste...

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Potential therapeutic applications of cannabinoids in gastrointestinal and liver diseases: Focus on Δ9‐tetrahydrocannabinol pharmacology

et al. 2014

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Effects of a cannabinoid receptor agonist on colonic motor and sensory functions in humans: a randomized, placebo-controlled study

Cited by 99 publications

References 32 publications

CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

Endogenous Cannabinoid System and Its Role in Gastrointestinal Tract: Review

Potential therapeutic applications of cannabinoids in gastrointestinal and liver diseases: Focus on Δ9‐tetrahydrocannabinol pharmacology

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Effects of a cannabinoid receptor agonist on colonic motor and sensory functions in humans: a randomized, placebo-controlled study

Cited by 99 publications

References 32 publications

CB1Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

CB1Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

Endogenous Cannabinoid System and Its Role in Gastrointestinal Tract: Review

Potential therapeutic applications of cannabinoids in gastrointestinal and liver diseases: Focus on Δ9‐tetrahydrocannabinol pharmacology

Contact Info

Product

Resources

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CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents

CB₁Receptors Mediate the Analgesic Effects of Cannabinoids on Colorectal Distension-Induced Visceral Pain in Rodents