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KISSMost common diseases are complex genetic traits. Identifying the genes that underlie the variation in the diseases has been challenging. Two major approaches have been used to map genetic variants that influence disease risk: linkage analysis and asso...
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RISS 인기검색어
https://www.riss.kr/link?id=A76550195
- 저자
- 발행기관
- 학술지명
- 권호사항
-
발행연도
2006
-
작성언어
-
- 주제어
-
KDC
500
-
등재정보
KCI등재,SCOPUS,ESCI
-
자료형태
학술저널
- 발행기관 URL
-
수록면
265-271(7쪽)
-
KCI 피인용횟수
0
- 제공처
-
0
상세조회 -
0
다운로드
부가정보
다국어 초록 (Multilingual Abstract)
Most common diseases are complex genetic traits. Identifying the genes that underlie the variation in the diseases has been challenging. Two major approaches have been used to map genetic variants that influence disease risk: linkage analysis and association study. Linkage analysis tests for the co-segregation of a marker and disease phenotype within a pedigree, whereas association study tests for differences in marker allele frequencies between patients and a control population. Linkage analysis is applied without any prior knowledge of the biological basis of the disease. In association study, genes with a known function with the potential to influence the disease phenotype are investigated for a direct role in disease. No single method is sufficient. A multi-strategy approach to the mapping of complex diseases is required. We review the different types of genetic studies to find genes for complex genetic traits.
Most common diseases are complex genetic traits. Identifying the genes that underlie the variation in the diseases has been challenging. Two major approaches have been used to map genetic variants that influence disease risk: linkage analysis and association study. Linkage analysis tests for the co-segregation of a marker and disease phenotype within a pedigree, whereas association study tests for differences in marker allele frequencies between patients and a control population. Linkage analysis is applied without any prior knowledge of the biological basis of the disease. In association study, genes with a known function with the potential to influence the disease phenotype are investigated for a direct role in disease. No single method is sufficient. A multi-strategy approach to the mapping of complex diseases is required. We review the different types of genetic studies to find genes for complex genetic traits.
참고문헌 (Reference)
1 "Variation is the spice of life" 27 : 234-236, 2001
2 "The genetics of complex autoimmune diseases:non-MHC susceptibility genes" 2 : 802-809, 2001
3 "The TDT and other family- based tests for linkage disequilibrium and association" 59 : 983-989, 1996
4 "Strategies in complex disease mapping" 10 : 330-334, 2000
5 "Strategies in analysis of the genetic component of multifactorial diseases;biostatistical aspects" 14 : 255-266, 2005
6 "Searching for genetic determinants in the new millennium" 405 : 847-856, 2000
7 "Rational inferences about departures from Hardy-Weinberg equilibrium" 76 : 967-986, 2005
8 "Proposed guidelines for papers describing DNA polymorphism- disease associations" 110 : 207-208, 2002
9 "Parametric and nonparametric linkage analysis:a uni-fied multipoint approach" 58 : 1347-1363, 1996
10 "New methods for finding disease-susceptibility genes:impact and potential" 4 : 119-, 2003
1 "Variation is the spice of life" 27 : 234-236, 2001
2 "The genetics of complex autoimmune diseases:non-MHC susceptibility genes" 2 : 802-809, 2001
3 "The TDT and other family- based tests for linkage disequilibrium and association" 59 : 983-989, 1996
4 "Strategies in complex disease mapping" 10 : 330-334, 2000
5 "Strategies in analysis of the genetic component of multifactorial diseases;biostatistical aspects" 14 : 255-266, 2005
6 "Searching for genetic determinants in the new millennium" 405 : 847-856, 2000
7 "Rational inferences about departures from Hardy-Weinberg equilibrium" 76 : 967-986, 2005
8 "Proposed guidelines for papers describing DNA polymorphism- disease associations" 110 : 207-208, 2002
9 "Parametric and nonparametric linkage analysis:a uni-fied multipoint approach" 58 : 1347-1363, 1996
10 "New methods for finding disease-susceptibility genes:impact and potential" 4 : 119-, 2003
11 "Identification of genes for a complex trait:examples from hypertension" 7 : 1-13, 2006
12 "How many diseases does it take to map a gene with SNPs" 26 : 151-157, 2000
13 "Hardy-Weinberg disequilibrium identified genotyping error of the serotonin transporter(SLC6A4)promoter polymorphism" 16 : 31-34, 2006
14 "Genomics and medicine.Dissecting human disease in the postgenomic era" 291 : 1224-1229, 2001
15 "Genomewide scans of complex human diseases:true linkage is hard to find" 69 : 936-950, 2001
16 "Genome-wide association studies for common diseases and complex traits" 6 : 95-108, 2005
17 "Genetic studies in complex disease:the case pro linkage studies" 1 : 1676-1678, 2003
18 "Genetic power calculator:design of linkage and association genetic mapping studies of complex traits" 19 : 149-150, 2003
19 "Genetic power calculator:design of linkage and association genetic mapping studies of complex traits" 19 : 149-150, 2003
20 "Genetic case-control association studies- correcting for multiple testing" 109 : 564-567, 2001
21 "Genetic case-control association studies correcting for multiple testing" 109 : 564-567, 2001
22 "Genetic association studies of complex traits:design and analysis issues" 573 : 54-69, 2005
23 "Genetic association mapping at the crossroads: which test and why? Overview and practical guidelines" 114 : 1-11, 2002
24 "Gene finding strategies" 61 : 53-71, 2002
25 "Finding genes that underlie complex traits" 298 : 2345-2349, 2002
26 "Comparison of statistical power between 2 * 2 allele frequency and allele positivity tables in case-control studies of complex disease genes" 65 : 197-206, 2001
27 "Case-control studies in the genomic era:a clinician's guide" 5 : 701-707, 2006
28 "Candidate gene case-control association studies:advantages and potential pitfalls" 52 : 489-499, 2001
29 "Association study designs for complex diseases" 2 : 91-99, 2001
30 "An overview of the genetic analysis of complex diseases,with reference to type 1 diabetes" 15 : 265-277, 2001
31 "A tutorial on statistical methods for population association studies" 7 : 781-791, 2006
32 "A revised estimate of twin concordance in systemic lupus erythematosus" 35 : 311-8, 1992
33 "A comprehensive review of genetic association studies" 4 : 45-61, 2002
34 "A clarification of the Hardy-Weinberg law" 174 : 1695-1697, 2006
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분석정보
인용정보 인용지수 설명보기
학술지 이력
| 연월일 | 이력구분 | 이력상세 | 등재구분 |
|---|---|---|---|
| 2027 | 평가예정 | 재인증평가 신청대상 (재인증) | |
| 2021-01-01 | 평가 | 등재학술지 유지 (재인증) |  |
| 2018-01-01 | 평가 | 등재학술지 유지 (등재유지) | |
| 2016-03-09 | 학회명변경 | 영문명 : The Korean Rheumatism Association -> Korean College of Rheumatology | |
| 2015-04-03 | 학술지명변경 | 외국어명 : The Journal of the Korean Rheumatism Association -> Journal of Rheumatic Diseases | |
| 2015-01-01 | 평가 | 등재학술지 유지 (등재유지) | |
| 2011-01-01 | 평가 | 등재학술지 유지 (등재유지) | |
| 2009-01-01 | 평가 | 등재학술지 유지 (등재유지) | |
| 2006-01-01 | 평가 | 등재학술지 선정 (등재후보2차) | |
| 2005-01-01 | 평가 | 등재후보 1차 PASS (등재후보1차) |  |
| 2003-01-01 | 평가 | 등재후보학술지 선정 (신규평가) | |
학술지 인용정보
| 기준연도 | WOS-KCI 통합IF(2년) | KCIF(2년) | KCIF(3년) |
|---|---|---|---|
| 2016 | 0.1 | 0.1 | 0.08 |
| KCIF(4년) | KCIF(5년) | 중심성지수(3년) | 즉시성지수 |
| 0.08 | 0.09 | 0.242 | 0.09 |
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