High-Throughput SNP Allele-Frequency Determination in Pooled DNA Samples by Kinetic PCR

Germer, Søren; Holland, Michael J.; Higuchi, Russell

doi:10.1101/gr.10.2.258

Cited by 396 publications

(306 citation statements)

References 42 publications

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“…no. M11810) was genotyped using allele-specific real-time PCR, which is a modified method according to Germer et al 34 Each reaction comprised 0.2 mM each of the primers specific for exon 8 ( ). An initial incubation step of 2 min at 501C (to allow UNG-mediated elimination of carryover PCR product contamination), and an enzyme heat activation step of 12 min at 951C were followed by 40 two-step amplification cycles of 20 s at 951C for denaturation and 20 s for 581C for annealing and extension, and a final 5 min extension at 721C.…”

Section: Genotyping Of Allelic Variantsmentioning

confidence: 99%

Polymorphisms in interferon-induced genes and the outcome of hepatitis C virus infection: roles of MxA, OAS-1 and PKR

et al. 2003

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Interferon stimulates the expression of a number of genes encoding enzymes with antiviral activities, including myxovirus resistance-1 (MxA), 2-5-oligoadenylate synthetase 1 (OAS-1) and double-stranded RNA-dependent protein kinase (PKR). We examined whether polymorphisms in these genes influenced the outcome of hepatitis C virus (HCV) infection. We observed a lower frequency of the GG genotype at position À88 in the MxA gene promoter in self-limiting HCV infection (OR ¼ 0.56; 95% CI: 0.35-0.8; P ¼ 0.010) and in nonresponders to therapy (OR ¼ 0.49; 95% CI: 0.25-0.95; P ¼ 0.020). This genotype predominantly influenced the outcome of treatment in patients with viral genotype 1 (OR ¼ 0.22 95% CI: 0.07-0.67; P ¼ 0.002). A polymorphism in the 3 0 -untranslated region of the OAS-1 gene was associated with outcome of infection (GG genotype less frequent in self-limiting infection: OR ¼ 0.43; 95% CI: 0.21-0.86; P ¼ 0.010). A polymorphism at position À168 in the promoter region of the PKR gene was associated with self-limiting infection (CT genotype: OR ¼ 2.75; 95% CI: 1.45-5.24; P ¼ 0.002). Further associations were found with a CGG trinucleotide repeat in the 5 0 UTR region of the PKR gene. Polymorphisms in the interferon-induced genes, MxA, OAS-1 and PKR appear thus associated with HCV outcome.

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Section: Genotyping Of Allelic Variantsmentioning

confidence: 99%

Polymorphisms in interferon-induced genes and the outcome of hepatitis C virus infection: roles of MxA, OAS-1 and PKR

et al. 2003

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“…For each individual, we genotyped the À173G/C promoter polymorphisms using the assay that combines kinetic (real-time quantitative) polymerase chain reaction (PCR) with allele-specific amplification in which primers were designed 30 (Primer Express software; PE Applied Biosystems, Foster City, CA, USA) to specifically amplify either the À173G or À173C allele in separate PCRs (À173G forward primer, 5 0 -CCGCCAAGTGGAGAA-CAGG-3 0 ; À173C forward primer, 5 0 -CCGCCAAGTGGA GAACAGC 3 0 ; À173G reverse primer, 5 0 -GGCGCACCG CTCCAAC-3 0 ; À173C reverse primer, 5 0 -GGCGCACCGC TCCAAG-3 0 ). The PCR products were detected using the ABI 7700 Sequence Detection System with a dsDNAspecific fluorescent dye SYBR Green I (PE Applied Biosystems).…”

Section: Screening For Mif Polymorphismmentioning

confidence: 99%

Promoter region polymorphism of macrophage migration inhibitory factor is strong risk factor for young onset of extensive alopecia areata

et al. 2005

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We have demonstrated that serum macrophage migration inhibitory factor (MIF) was significantly elevated in patients with extensive alopecia areata (AA). Recently, functional polymorphisms have been identified in the MIF promoter region. To address the functional and prognostic relevance of the À173G/C and À794[CATT] 5-8 repeat polymorphisms in MIF genes in patients with extensive AA, 113 patients with extensive AA and 194 healthy controls were genotyped. We found that MIFÀ173*C was a risk factor for early onset (o20 years) of extensive AA (odds ratio for GC heterozygotes with À173G/C was 4.88 (95% CI, 2.04-11.8), P ¼ 0.00038; odds ratio for CC homozygotes with À173G/C was 10.42 (95% CI, 2.56-43.5), P ¼ 0.0011). We found no statistically significant differences in the genotype frequencies of the À794[CATT] 5-8 repeat polymorphism and extensive AA. These results suggest that polymorphisms within the MIFÀ173*C allele confer an increased risk of susceptibility to the extensive forms of AA, especially with an early onset of disease. MIF is therefore suggested to be closely implicated in the pathogenesis of the more extensive forms of AA.

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“…The assay used in this study combines kinetic (real-time quantitative) PCR with allele-specific amplification, which has been described elsewhere. 15 PCR primers used in this study were designed by a tetra-primer ARMS-PCR primer design program. Only one outer primer and inner primer pair was chosen for PCR from the four output primers.…”

Section: Genotypingmentioning

confidence: 99%

Family-based association study of Epsin 4 and Schizophrenia

et al. 2006

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Recently, Pimm et al. identified Epsin 4 on chromosome 5q33 as a susceptibility gene for schizophrenia in the British population, based on linkage and association evidence. In Pimm's case-control study, both the single polymorphisms and the individual haplotypes at the 5 0 end of the gene showed genetic association with schizophrenia. Here, we report the first study evaluating the relevance of Epsin 4 and schizophrenia outside the British population. Markers showing positive results in the original work as well as two additional polymorphisms were genotyped in 308 Han Chinese family trios. Transmission disequilibrium analysis was used to test for association of single-locus markers and multi-locus haplotypes with schizophrenia. Although no individual marker was significant at the P = 0.05 level, the haplotypes detected in our samples, different from those previously reported, showed strong evidence of association (most significant global P = 0.0021). Our results indicate the presence of a locus near the 5 0 end of Epsin 4 conferring susceptibility to the disease and provide further support for Epsin 4 as an important potential contributor to genetic risk in schizophrenia.

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High-Throughput SNP Allele-Frequency Determination in Pooled DNA Samples by Kinetic PCR

Cited by 396 publications

References 42 publications

Polymorphisms in interferon-induced genes and the outcome of hepatitis C virus infection: roles of MxA, OAS-1 and PKR

Polymorphisms in interferon-induced genes and the outcome of hepatitis C virus infection: roles of MxA, OAS-1 and PKR

Promoter region polymorphism of macrophage migration inhibitory factor is strong risk factor for young onset of extensive alopecia areata

Family-based association study of Epsin 4 and Schizophrenia

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