Platelet-activating factor acetylhydrolase deficiency. A missense mutation near the active site of an anti-inflammatory phospholipase.

Stafforini, Diana M.; Satoh, Kei; Atkinson, Donald L.; Tjoelker, Larry W.; Eberhardt, Chris; Yoshida, Hidemi; Imaizumi, Tada Atsu; Takamatsu, Shigeru; Zimmerman, Guy A.; McIntyre, Thomas M.; Gray, Patrick W.; Prescott, Stephen M.

doi:10.1172/jci118733

Cited by 255 publications

(201 citation statements)

References 42 publications

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“…Concerning platelet membrane glycoproteins, it has been reported that genetic polymorphisms of GPIa, 10 GPIba, 11 GPIIIa 12,13 and GPVI 14 influence the efficacy of aspirin or platelet responsiveness. Furthermore, Halushka et al 15 reported the association of platelet aggregation with genetic mutation of COX-1, Papafili et al 16 the association with genetic mutation of COX-2, Higuchi et al 17 the association with genetic mutation of TXA 2 receptors (TP), Stafforini et al 18 the association with genetic mutation of platelet activating factor acetylhydrolase (PAFAH) and Undas et al 19 the association with genetic mutation of coagulation factor XIII (FXIII).…”

Section: Introductionmentioning

confidence: 99%

Exploratory aspirin resistance trial in healthy Japanese volunteers (J-ART) using platelet aggregation as a measure of thrombogenicity

et al. 2007

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Section: Introductionmentioning

confidence: 99%

Exploratory aspirin resistance trial in healthy Japanese volunteers (J-ART) using platelet aggregation as a measure of thrombogenicity

et al. 2007

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“…The Val279Phe (V279F) homogygous mutation (279FF) is the only polymorphism theoretically resulting in no circulating gene product of Lp-PLA2. 9, 10 The prevalence of 279FF was reported to be 0.4%, 1.2%, and 3% in the Chinese, Korean, and Japanese populations, respectively, 11-13 but this variant is rare in non-Asian populations. 14 In a recent meta-analysis including 79,036 participants in 32 prospective studies, Lp-PLA2 activity and mass each showed continuous associations with risk of CAD, similar in magnitude to that with non-high-density lipoprotein cholesterol and systolic blood pressure.…”

Section: Discussionmentioning

confidence: 99%

“…9, 10 Jang et al found that the V279F variant in the PLA2G7 gene led to significant loss of enzyme activity in heterozygous subjects and no appreciable enzyme activity in homozygous subjects. The mechanism of the deficiencies of plasma Lp-PLA2 activity were suggested to be due to a loss-of-function mutation (V279F, exon 9, position 994; G3T; G>T) in the Lp-PLA2 gene, because Val-279 conserved in plasma Lp-PLA2 lies between the active site Ser-273 and Asp-296 residues in a region that is critical for proper folding of the enzyme.…”

Section: Efficacymentioning

confidence: 99%

“…12 It has been reported that the mutant allele was present in 27% of the Japanese population as heterozygotes and in 4% as homozygotes. 10 In contrast, no heterozygous or homozygous deficient subjects were identified in a random North American population 10 and were rare in the Caucasian hapmap samples and absent in the African samples (www.hapmap.org). In addition, some reports showed that Lp-PLA2 activity in the 279VF population was approximately half of that in the 279VV population, and that 279FF completely lacked Lp-PLA2 activity.…”

Section: Efficacymentioning

confidence: 99%

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Effect of Darapladib on Plasma Lipoprotein-Associated Phospholipase A2 Activity in Japanese Dyslipidemic Patients, With Exploratory Analysis of a PLA2G7 Gene Polymorphism of Val279Phe

Daida

Iwase

Yagi

et al. 2013

Circ J

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“…Stafforini et al 19 mapped the PLA2G7 gene (PAFAH) to chromosome 6p21.1-p12 and found that it contains 12 exons. Deficiency of plasma platelet-activating factor resulting from a missense mutation (Val279-Phe) in exon 9 of the gene has been described.…”

mentioning

confidence: 99%

Study of association between genetic polymorphisms of phospholipase A2 enzymes and Alzheimer's disease

Cordeiro

Noguti

Bottino

et al. 2010

Arq. Neuro-Psiquiatr.

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Several genes have been related to late-onset Alzheimer's disease (LOAD). Phospholipases A2 (PLA2) influence the processing and secretion of the amyloid precursor protein, which gives rise to the beta-amyloid peptide, the major component of the amyloid plaque in AD. Hence, in the present study, polymorphisms of three genes encoding PLA2 enzymes group (cytosolic PLA2: BanI cPLA2 polymorphism; calcium-independent PLA2: AvrII iPLA2 polymorphism; PAFAH: Val279Phe PAFAH polymorphism) were analysed in a case-control sample using 58 patients with LOAD and 107 matched healthy controls. There was a genotypic association between the BanI cPLA2 polymorphism and LOAD (c 2 =6.25, 2df, p=0.04), however there was no allelic association. There were no associations between AvrII iPLA2 and Val279Phe PAFAH polymorphisms and LOAD. These data suggest that the BanI cPLA2 polymorphism may play a role in the susceptibility for LOAD in our Brazilian sample. Key words: PLA2, dementia, gene, genetics, LOAD.Associação entre polimorfismos das enzimas fosfolipases A2 e doença de Alzheimer resumo Vários genes têm sido investigados como fatores de risco para o desenvolvimento da doença de Alzheimer (DA) de início tardio. As fosfolipases A2 (PLA2) influenciam o processamento e secreção da proteína precursora do amilóide, que dá origem ao peptídeo meta-amilóide, o principal componente da placa amilóide na DA. Assim, no presente estudo, foram analisados três polimorfismos genéticos que codificam enzimas do grupo das PLA2 (PLA2 citosólica: polimorfismo BanI cPLA2; PLA2 cálcio-independente: polimorfismo AvrII iPLA2; PAFAH: polimorfismo Val279Phe PAFAH) em 58 pacientes com DA de início tardio e 107 controles saudáveis pareados. Houve associação genotípica entre o polimorfismo BanI cPLA2 e DA de início tardio (c 2 =6,25, 2df, p=0,04); no entanto não foi observada associação alélica. Não houve associação entre os polimorfismos AvrII iPLA2 e Val279Phe PAFAH com a doença. Tais dados sugerem que o polimorfismo BanI cPLA2 pode estar envolvido como fator de susceptibilidade para DA de início tardio em nossa amostra brasileira. Palavras-chave: PLA2, demência, gene, genética, Alzheimer de início tardio.

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Platelet-activating factor acetylhydrolase deficiency. A missense mutation near the active site of an anti-inflammatory phospholipase.

Cited by 255 publications

References 42 publications

Exploratory aspirin resistance trial in healthy Japanese volunteers (J-ART) using platelet aggregation as a measure of thrombogenicity

Exploratory aspirin resistance trial in healthy Japanese volunteers (J-ART) using platelet aggregation as a measure of thrombogenicity

Effect of Darapladib on Plasma Lipoprotein-Associated Phospholipase A<sub>2</sub> Activity in Japanese Dyslipidemic Patients, With Exploratory Analysis of a <i>PLA<sub>2</sub>G7</i> Gene Polymorphism of Val279Phe

Study of association between genetic polymorphisms of phospholipase A2 enzymes and Alzheimer's disease

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