Deep sequencing analysis to identify novel and rare variants in pain-related genes in patients with acute postoperative pain and high morphine use

Most of the genetic variants that are reported to be associated with common pain phenotypes and analgesic use are common polymorphisms. The objective of our study was to identify new variants and investigate less common genetic variants that are usually not included in either small single-gene studi...

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Published inJournal of pain research Vol. 12; pp. 2755 - 2770
Main Authors Loke, Mun-Fai, Wei, Heming, Yeo, Junjie, Sng, Ban-Leong, Sia, Alex T, Tan, Ene-Choo
Format Journal Article
LanguageEnglish
Published New Zealand Dove Medical Press Limited 01.09.2019
Taylor & Francis Ltd
Dove
Dove Medical Press
Subjects
Analysis
Asians
Care and treatment
Chronic illnesses
Deflation (Economics)
Deoxyribonucleic acid
DNA
Dopamine
EDTA
Genes
Genetic aspects
genetic variants
Genomes
Genomics
Hospitals
Hysterectomy
Medical research
Morphine
Mutation
next-generation sequencing (NGS)
Novels
Original Research
Pain
Patients
Peptides
Phenotypes
Postoperative pain
RNA
Studies
Surgery
Twins
Singapore
United States > US
genetic variants
next-generation sequencing
postoperative pain
morphine
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Summary:Most of the genetic variants that are reported to be associated with common pain phenotypes and analgesic use are common polymorphisms. The objective of our study was to identify new variants and investigate less common genetic variants that are usually not included in either small single-gene studies or high-throughput genotyping arrays. From a cohort of 1075 patients who underwent a scheduled total abdominal hysterectomy, 92 who had higher self-rated pain scores and used more morphine were selected for the re-sequencing of 105 genes. We identified over 2400 variants in 104 genes. Most were intronic with frequencies >5%. There were 181 novel variants, of which 30 were located in exons: 17 nonsynonymous, 10 synonymous, 2 non-coding RNA, and 1 stop-gain. For known variants that are rare (population frequency <1%), the frequencies of 54 exonic variants and eight intronic variants for the sequenced samples were higher than the weighted frequencies in the Genome Aggregation Database for East and South Asians ( -values ranging from 0.000 to 0.046). Overall, patients who had novel and/or rare variants used more morphine than those who only had common variants. Our study uncovered novel variants in patients who reported higher pain and used more morphine. Compared with the general population, rare variants were more common in this group.
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ISSN:1178-7090
1178-7090
DOI:10.2147/JPR.S213869