Association of OPRM1 A118G variant with risk of morphine-induced respiratory depression following spine fusion in adolescents

Chidambaran, Vidya; Mavi, Jagroop; Esslinger, Hope; Pilipenko, Valentina; Martin, Lisa J.; Zhang, K; Sadhasivam, Senthilkumar

doi:10.1038/tpj.2014.59

Cited by 37 publications

(31 citation statements)

References 51 publications

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“…Twin studies have revealed significant heritability (30%) for RD from opioids [62]; contributing nongenetic risk factors like female sex and medical comorbidities have been described [63][64][65]. Our study strengthens the evidence for FAAH associations with morphine outcomes in children, adds to the genetic risk factors reported previously -OPRM1 [66] and ABCB1 [67] and expands the knowledge base toward identifying genetic risk signatures for RD in children [68]. FAAH inhibitors have been explored for treatment of pain and nausea [69,70]; our findings spur further investigation of these agents to alter risk of opioid RD.…”

Section: Discussionsupporting

confidence: 76%

Fatty Acid Amide Hydrolase–morphine Interaction Influences Ventilatory Response to Hypercapnia and Postoperative Opioid Outcomes in Children

et al. 2016

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Aim: Fatty acid amide hydrolase (FAAH) degrades anandamide, an endogenous cannabinoid. We hypothesized that FAAH variants will predict risk of morphine-related adverse outcomes due to opioid-endocannabinoid interactions. Patients & methods:In 101 postsurgical adolescents receiving morphine analgesia, we prospectively studied ventilatory response to 5% CO 2 (HCVR), respiratory depression (RD) and vomiting. Blood was collected for genotyping and morphine pharmacokinetics. Results: We found significant FAAH-morphine interaction for missense (rs324420) and several regulatory variants, with HCVR (p < 0.0001) and vomiting (p = 0.0339). HCVR was more depressed in patients who developed RD compared with those who did not (p = 0.0034), thus FAAH-HCVR association predicts risk of impending RD from morphine use. Conclusion: FAAH genotypes predict risk for morphine-related adverse outcomes.

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Section: Discussionsupporting

confidence: 76%

Fatty Acid Amide Hydrolase–morphine Interaction Influences Ventilatory Response to Hypercapnia and Postoperative Opioid Outcomes in Children

et al. 2016

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“…However, the use of morphine is at risk of addiction and respiratory depression (Chidambaran et al 2015). Many physicians and patients are reluctant to use morphine for fear of respiratory depression and the lack of comprehensive understanding about morphine.…”

Section: Discussionmentioning

confidence: 99%

Morphine versus methylprednisolone or aminophylline for relieving dyspnea in patients with advanced cancer in China: a retrospective study

Tian

Wang

et al. 2016

SpringerPlus

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ContextDyspnea is one of the most common and distressing symptoms that occurs in terminal cancer patients. However, there are no existing treatment guidelines for this condition in China.ObjectiveThis single-center, retrospective, observational study aimed to compare the efficacy of using morphine, methylprednisolone, or aminophylline to relieve the symptom of breathlessness in patients with advanced malignant tumors and to investigate the safety of these regimens during the treatment of dyspnea.MethodsBetween August 2011 and January 2015 we retrospectively reviewed the medical records of 343 terminally ill cancer patients with dyspnea who received morphine, methylprednisolone, or aminophylline. The therapeutic effect of each treatment by means of visual analogue scale (VAS) scores was assessed and compared. Statistical methods included Chi square and analysis of variance tests. Differences were considered significant when P < 0.05.ResultsVAS scores after treatment were (16.82 ± 10.89), (25.72 ± 15.03), and (31.95 ± 16.00) points in the morphine, methylprednisolone, and aminophylline group, respectively. These differences were found to be significantly different (P < 0.05). The effectiveness ratings were 86.44, 62.16, and 49.12%, respectively (P < 0.05).ConclusionsWe found that morphine subcutaneous injection for advanced cancer patients with dyspnea was safe and typically more effective than methylprednisolone or aminophylline. Therefore, morphine treatment could significantly improve the quality of life in terminal cancer patients with short life expectancies who are experiencing shortness of breath.

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“…This mutation leads to decreased cell surface expression and overall receptor stability combined with more subtle effects on the binding affinity of opioid peptides and small molecules (69,70). Increasing evidence suggests that this variant may alter pain threshold levels, sensitivity to clinically used opioids, and risk of opioidinduced respiratory depression (71)(72)(73). At a structural level, the direct consequence of this variant remains unknown owing to truncations in the presumably flexible amino terminus required for crystallography.…”

Section: Genetic Variation In Opioid Receptor Structurementioning

confidence: 99%

Molecular Basis of Opioid Action: From Structures to New Leads

Manglik

2020

Biological Psychiatry

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Since the isolation of morphine from the opium poppy over 200 years ago, the molecular basis of opioid action has remained the subject of intense inquiry. The identification of specific receptors responsible for opioid function and the discovery of many chemically diverse molecules with unique opioid-like efficacies have provided glimpses into the molecular logic of opioid action. Recent revolutions in the structural biology of transmembrane proteins have, for the first time, yielded high-resolution views into the 3-dimensional shapes of all 4 opioid receptors. These studies have begun to decode the chemical logic that enables opioids to specifically bind and activate their receptor targets. A combination of spectroscopic experiments and computational simulations has provided a view into the molecular movements of the opioid receptors, which itself gives rise to the complex opioid pharmacology observed at the cellular and behavioral levels. Further diversity in opioid receptor structure is driven by both genetic variation and receptor oligomerization. These insights have enabled computational drug discovery efforts, with some evidence of success in the design of completely novel opioids with unique efficacies. The combined progress over the past few years provides hope for new, efficacious opioids devoid of the side effects that have made them the scourge of humanity for millennia.

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Association of OPRM1 A118G variant with risk of morphine-induced respiratory depression following spine fusion in adolescents

Cited by 37 publications

References 51 publications

Fatty Acid Amide Hydrolase–morphine Interaction Influences Ventilatory Response to Hypercapnia and Postoperative Opioid Outcomes in Children

Fatty Acid Amide Hydrolase–morphine Interaction Influences Ventilatory Response to Hypercapnia and Postoperative Opioid Outcomes in Children

Morphine versus methylprednisolone or aminophylline for relieving dyspnea in patients with advanced cancer in China: a retrospective study

Molecular Basis of Opioid Action: From Structures to New Leads

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