Screening for pain phenotypes: Analysis of three congenic mouse strains on a battery of nine nociceptive assays
In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains – in which a small portion of the genome of the MOLF/Ei strain has been placed on a C57BL/6 genetic background – on a battery of nine nociceptive assays, chosen to reflect thos...
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Published in | Pain (Amsterdam) Vol. 126; no. 1; pp. 24 - 34 |
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Main Authors | , , , , , , |
Format | Journal Article |
Language | English |
Published |
Amsterdam
Elsevier B.V
15.12.2006
Elsevier |
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Abstract | In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains – in which a small portion of the genome of the MOLF/Ei strain has been placed on a C57BL/6 genetic background – on a battery of nine nociceptive assays, chosen to reflect those assays in most common use in the pain literature. Mice of both sexes were evaluated by two different testers at different points in time, allowing us to examine the relative importance of genotype, sex, tester and cohort effects on data from these assays. We find strong evidence for the existence of two quantitative trait loci (i.e., genomic regions containing variability-causing genes), one for thermal nociception on mouse chromosome (Chr) 17 (Chr 17;
Tpnr3) and one for formalin test nociception on mouse Chr 12 (
Nociq3). We note, however, that the nociceptive assays in this battery feature strong main effects and interactions of sex, tester, and cohort, which if not controlled or covaried can seriously confound interpretation of genetic experiments, including the comparison of transgenic knockout mice to their wild-type controls. |
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AbstractList | In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains--in which a small portion of the genome of the MOLF/Ei strain has been placed on a C57BL/6 genetic background--on a battery of nine nociceptive assays, chosen to reflect those assays in most common use in the pain literature. Mice of both sexes were evaluated by two different testers at different points in time, allowing us to examine the relative importance of genotype, sex, tester and cohort effects on data from these assays. We find strong evidence for the existence of two quantitative trait loci (i.e., genomic regions containing variability-causing genes), one for thermal nociception on mouse chromosome (Chr) 17 (Chr 17; Tpnr3) and one for formalin test nociception on mouse Chr 12 (Nociq3). We note, however, that the nociceptive assays in this battery feature strong main effects and interactions of sex, tester, and cohort, which if not controlled or covaried can seriously confound interpretation of genetic experiments, including the comparison of transgenic knockout mice to their wild-type controls. In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains – in which a small portion of the genome of the MOLF/Ei strain has been placed on a C57BL/6 genetic background – on a battery of nine nociceptive assays, chosen to reflect those assays in most common use in the pain literature. Mice of both sexes were evaluated by two different testers at different points in time, allowing us to examine the relative importance of genotype, sex, tester and cohort effects on data from these assays. We find strong evidence for the existence of two quantitative trait loci (i.e., genomic regions containing variability-causing genes), one for thermal nociception on mouse chromosome (Chr) 17 (Chr 17; Tpnr3) and one for formalin test nociception on mouse Chr 12 ( Nociq3). We note, however, that the nociceptive assays in this battery feature strong main effects and interactions of sex, tester, and cohort, which if not controlled or covaried can seriously confound interpretation of genetic experiments, including the comparison of transgenic knockout mice to their wild-type controls. |
Author | Mogil, Jeffrey S. Croteau, Sylvie Ritchie, Jennifer Levitin, Daniel J. Sotocinal, Susana G. Smith, Shad B. Naumova, Anna K. |
Author_xml | – sequence: 1 givenname: Jeffrey S. surname: Mogil fullname: Mogil, Jeffrey S. email: jeffrey.mogil@mcgill.ca organization: Department of Psychology and Centre for Research on Pain, McGill University, Montreal, Que., Canada – sequence: 2 givenname: Jennifer surname: Ritchie fullname: Ritchie, Jennifer organization: Department of Psychology and Centre for Research on Pain, McGill University, Montreal, Que., Canada – sequence: 3 givenname: Susana G. surname: Sotocinal fullname: Sotocinal, Susana G. organization: Department of Psychology and Centre for Research on Pain, McGill University, Montreal, Que., Canada – sequence: 4 givenname: Shad B. surname: Smith fullname: Smith, Shad B. organization: Department of Psychology and Centre for Research on Pain, McGill University, Montreal, Que., Canada – sequence: 5 givenname: Sylvie surname: Croteau fullname: Croteau, Sylvie organization: Department of Obstetrics and Gynecology, Research Institute of McGill University Health Centre, Montreal, Que., Canada – sequence: 6 givenname: Daniel J. surname: Levitin fullname: Levitin, Daniel J. organization: Department of Psychology and Centre for Research on Pain, McGill University, Montreal, Que., Canada – sequence: 7 givenname: Anna K. surname: Naumova fullname: Naumova, Anna K. organization: Department of Obstetrics and Gynecology, Research Institute of McGill University Health Centre, Montreal, Que., Canada |
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Keywords | Nociception QTL Genetics Algesiometry Sex difference Tester effects Pain sensitivity Interaction Variability Rodentia Sex Genotype Interpretation Strain Vertebrata Phenotype Mammalia Pain Mouse |
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Snippet | In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains – in which a small portion of the... In an attempt to identify new genes responsible for variability in pain sensitivity, we tested three congenic mouse strains--in which a small portion of the... |
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SubjectTerms | Algesiometry Animals Biological and medical sciences Chromosome Mapping Female Formaldehyde Fundamental and applied biological sciences. Psychology Genetics Genotype Hot Temperature Illness and personality Illness, stress and coping Male Mice Mice, Congenic Nociception Nociceptors - physiology Pain - chemically induced Pain - etiology Pain - genetics Pain - physiopathology Pain Threshold - physiology Phenotype Psychology and medicine Psychology. Psychoanalysis. Psychiatry Psychology. Psychophysiology QTL Quantitative Trait Loci Sex difference Sex Factors Somesthesis and somesthetic pathways (proprioception, exteroception, nociception); interoception; electrolocation. Sensory receptors Tester effects Vertebrates: nervous system and sense organs |
Title | Screening for pain phenotypes: Analysis of three congenic mouse strains on a battery of nine nociceptive assays |
URI | https://dx.doi.org/10.1016/j.pain.2006.06.004 https://www.ncbi.nlm.nih.gov/pubmed/16842916 |
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