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Vol. 293, Issue 1, 180-187, April 2000
Department of Behavioral Neuroscience, Oregon Health Sciences
University, and Research Service, Veterans Affairs Medical Center,
Portland, Oregon
Seizures are a well known consequence of human cocaine abuse, and in
rodent models, sensitivity to cocaine seizures has been shown to be
strongly influenced by genotype. For example, several studies have
reported significant differences between the C57BL/6 (B6) and DBA/2
(D2) inbred mouse strains in their sensitivity to cocaine-induced
seizures. This prompted our use of the BXD recombinant inbred
(RI) strain set and an F2 population derived from the B6
and D2 progenitor strains for further genetic analyses and for gene
mapping efforts in this study. Cocaine was infused into the lateral
tail vein, and the doses needed to induce a running bouncing clonic
seizure and a tonic hindlimb extensor seizure were recorded for each
mouse. In the BXD RI set, a genome-wide search was carried out for QTLs
(quantitative trait loci), which are sites on a chromosome containing
genes that influence seizure susceptibility. An F2
population (B6D2F2, n = 408) was subsequently used
as a second, confirmation step. Based on both RI and F2
results, three QTLs emerged as significant (P < .00005): one for clonic seizures on chromosome 9 (distal), and two for
tonic seizures on chromosomes 14 (proximal to mid) and 15 (distal). Two
additional QTLs emerged as suggestive (P < .0015),
both associated with clonic seizures on chromosomes 9 (proximal) and 15 (distal). Both QTLs on chromosome 9 were sex-specific, with much larger
effects on the phenotype seen in females than in males.
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