FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2733487544> ?p ?o ?g. }

• W2733487544 endingPage "41" @default.
• W2733487544 startingPage "32" @default.
• W2733487544 abstract "Purpose: Dementia is a multifactorial idiopathic pathology caused by clinical, eDementia is a multifactorial idiopathic pathology caused by clinical, environmental and genetic factors. Hence, its etiology is still unknown. We aimed to evaluate the association between five genetic risk factors for vascular diseases and dementia individually and when gathered in haplotypes. Materials and Method: We enrolled 200 dementia patients and 300 controls. All subjects were genotyped for vascular diseaseassociated polymorphisms in the genes coding for Apolipoprotein-E (ApoE), angiotensin converting enzyme (ACE) and Paraoxonase-1 (PON1). Results: The association between dementia risk and all the studied polymorphisms except of PON1-Q192R was found to be significant. Carrying the ApoE e4 allele seems to increase dementia risk by 4.32 fold (p = 0.001). The risk associated with ACE I and PON1-L55M T alleles were lower (2.58 and 2.11 fold, p < 0.001 and p = 0.015, respectively). When combined in haplotypes, these polymorphisms showed a cumulative and synergetic effect. GTICC haplotype appears to be associated with 9-fold dementia risk (p < 0.001), whereas AADTT seems to reduce dementia risk by 80% (p = 0.003). Conclusion: Our results suggest that, ApoE ε4, ACE I and PON1-L55M T alleles are associated with dementia risk whether these polymorphisms were studied separately or gathered in haplotypes. Still, the contribution of each gene to the pathophysiological development of dementia must be more investigated." @default.
• W2733487544 created "2017-07-14" @default.
• W2733487544 creator A5001322535 @default.
• W2733487544 creator A5006364150 @default.
• W2733487544 creator A5021268078 @default.
• W2733487544 creator A5038562050 @default.
• W2733487544 creator A5049729251 @default.
• W2733487544 creator A5053644491 @default.
• W2733487544 creator A5061504313 @default.
• W2733487544 creator A5062329373 @default.
• W2733487544 creator A5064973277 @default.
• W2733487544 creator A5085317148 @default.
• W2733487544 creator A5008593919 @default.
• W2733487544 creator A5074418434 @default.
• W2733487544 date "2017-07-16" @default.
• W2733487544 modified "2023-09-27" @default.
• W2733487544 title "Association between dementia and vascular disease-associated polymorphisms in a Tunisian population" @default.
• W2733487544 cites W1179757862 @default.
• W2733487544 cites W1569630040 @default.
• W2733487544 cites W1643500256 @default.
• W2733487544 cites W1647610000 @default.
• W2733487544 cites W1669374546 @default.
• W2733487544 cites W1729585270 @default.
• W2733487544 cites W1968630368 @default.
• W2733487544 cites W1973342161 @default.
• W2733487544 cites W1974560117 @default.
• W2733487544 cites W1976446430 @default.
• W2733487544 cites W1978065874 @default.
• W2733487544 cites W1984827465 @default.
• W2733487544 cites W1986457413 @default.
• W2733487544 cites W1995037165 @default.
• W2733487544 cites W1998316762 @default.
• W2733487544 cites W1998959104 @default.
• W2733487544 cites W1999061258 @default.
• W2733487544 cites W1999511995 @default.
• W2733487544 cites W2002821331 @default.
• W2733487544 cites W2002877822 @default.
• W2733487544 cites W2012611625 @default.
• W2733487544 cites W2014359105 @default.
• W2733487544 cites W2014874996 @default.
• W2733487544 cites W2018066652 @default.
• W2733487544 cites W2019077981 @default.
• W2733487544 cites W2025668878 @default.
• W2733487544 cites W2026928182 @default.
• W2733487544 cites W2034681842 @default.
• W2733487544 cites W2039857463 @default.
• W2733487544 cites W2042755992 @default.
• W2733487544 cites W2044451567 @default.
• W2733487544 cites W2044936845 @default.
• W2733487544 cites W2045930196 @default.
• W2733487544 cites W2045964495 @default.
• W2733487544 cites W2046703030 @default.
• W2733487544 cites W2051765035 @default.
• W2733487544 cites W2054502487 @default.
• W2733487544 cites W2058198277 @default.
• W2733487544 cites W2060460169 @default.
• W2733487544 cites W2061916198 @default.
• W2733487544 cites W2064552352 @default.
• W2733487544 cites W2065428558 @default.
• W2733487544 cites W2070654288 @default.
• W2733487544 cites W2071736632 @default.
• W2733487544 cites W2077595053 @default.
• W2733487544 cites W2078002929 @default.
• W2733487544 cites W2078526277 @default.
• W2733487544 cites W2080123209 @default.
• W2733487544 cites W2081716769 @default.
• W2733487544 cites W2082411752 @default.
• W2733487544 cites W2099720133 @default.
• W2733487544 cites W2110174245 @default.
• W2733487544 cites W2114751358 @default.
• W2733487544 cites W2116409842 @default.
• W2733487544 cites W2117913633 @default.
• W2733487544 cites W2118094114 @default.
• W2733487544 cites W2121101037 @default.
• W2733487544 cites W2124727440 @default.
• W2733487544 cites W2128387720 @default.
• W2733487544 cites W2128963466 @default.
• W2733487544 cites W2136932227 @default.
• W2733487544 cites W2137482821 @default.
• W2733487544 cites W2137903730 @default.
• W2733487544 cites W2139935881 @default.
• W2733487544 cites W2140718540 @default.
• W2733487544 cites W2141671076 @default.
• W2733487544 cites W2141820415 @default.
• W2733487544 cites W2143955562 @default.
• W2733487544 cites W2145291157 @default.
• W2733487544 cites W2146211420 @default.
• W2733487544 cites W2151217555 @default.
• W2733487544 cites W2156220037 @default.
• W2733487544 cites W2157131586 @default.
• W2733487544 cites W2159988524 @default.
• W2733487544 cites W2163267648 @default.
• W2733487544 cites W2329157757 @default.
• W2733487544 cites W2329901314 @default.
• W2733487544 cites W2461395267 @default.
• W2733487544 cites W2616596266 @default.
• W2733487544 cites W3190948865 @default.
• W2733487544 doi "https://doi.org/10.1080/00207454.2017.1348353" @default.

• next