TY - JOUR
T1 - Cross-sectional assessment of the consequences of a GTP cyclohydrolase 1 haplotype for specialized tertiary outpatient pain care
AU - Doehring, Alexandra
AU - Freynhagen, Rainer
AU - Griessinger, Norbert
AU - Zimmermann, Michael
AU - Sittl, Reinhard
AU - Hentig, Nils Von
AU - Geisslinger, Gerd
AU - Lötsch, Jörn
PY - 2009
Y1 - 2009
N2 - OBJECTIVES: Reduced-function variants of the guanosine triphosphate cyclohydrolase gene (GCH1) have been associated with reduced pain in well-defined cohorts of patients and healthy volunteers. We addressed the question whether this genetic association plays a role in outpatient pain therapy. METHODS: In a cross-sectional observational study, 523 patients were enrolled in 3 different tertiary care outpatient pain centers at German University hospitals. Of the 519 Caucasian patients, data from 424 could be analyzed for functional associations of the formerly named pain-protective GCH1 haplotype with the key characteristics of pain therapy being (1) actual pain, (2) opioid dosing, and (3) pain therapy duration. RESULTS: With an allelic frequency of 14.2% the pain-protective haplotype was not rarer among pain patients than in the general population (P=0.344). However, a tendency toward gene dose-dependent effects of the GCH1 haplotype was observed in all the 3 therapy parameters. Carriers of the haplotype tended to have lower actual 24-hour pain scores (n=424; P=0.18), require lower opioid doses (P=0.096), and were significantly shorter on specialized pain therapy (P=0.004). The latter applied predominantly to differences between homozygous carriers and heterozygous (α-corrected t test: P=0.06) or non-carriers (P=0.011) of the haplotype. CONCLUSIONS: The results strength the support for a modest yet reproducible and consistent pain-protective effect associated with a GCH1 haplotype known to reduce GCH1 and thus BH4 up-regulation. Pending independent verification, the results might point to a prophylactic role of decreased GCH1 up-regulation delaying the need for pain therapy.
AB - OBJECTIVES: Reduced-function variants of the guanosine triphosphate cyclohydrolase gene (GCH1) have been associated with reduced pain in well-defined cohorts of patients and healthy volunteers. We addressed the question whether this genetic association plays a role in outpatient pain therapy. METHODS: In a cross-sectional observational study, 523 patients were enrolled in 3 different tertiary care outpatient pain centers at German University hospitals. Of the 519 Caucasian patients, data from 424 could be analyzed for functional associations of the formerly named pain-protective GCH1 haplotype with the key characteristics of pain therapy being (1) actual pain, (2) opioid dosing, and (3) pain therapy duration. RESULTS: With an allelic frequency of 14.2% the pain-protective haplotype was not rarer among pain patients than in the general population (P=0.344). However, a tendency toward gene dose-dependent effects of the GCH1 haplotype was observed in all the 3 therapy parameters. Carriers of the haplotype tended to have lower actual 24-hour pain scores (n=424; P=0.18), require lower opioid doses (P=0.096), and were significantly shorter on specialized pain therapy (P=0.004). The latter applied predominantly to differences between homozygous carriers and heterozygous (α-corrected t test: P=0.06) or non-carriers (P=0.011) of the haplotype. CONCLUSIONS: The results strength the support for a modest yet reproducible and consistent pain-protective effect associated with a GCH1 haplotype known to reduce GCH1 and thus BH4 up-regulation. Pending independent verification, the results might point to a prophylactic role of decreased GCH1 up-regulation delaying the need for pain therapy.
KW - GCH1 haplotype
KW - Genetics
KW - Outpatient
KW - Pain therapy
UR - http://www.scopus.com/inward/record.url?scp=72149086459&partnerID=8YFLogxK
U2 - 10.1097/AJP.0b013e3181b43e12
DO - 10.1097/AJP.0b013e3181b43e12
M3 - Article
C2 - 19851158
AN - SCOPUS:72149086459
SN - 0749-8047
VL - 25
SP - 781
EP - 785
JO - Clinical Journal of Pain
JF - Clinical Journal of Pain
IS - 9
ER -