Literature DB >> 9222966

Genetic linkage study of familial Mediterranean fever (FMF) to 16p13.3 and evidence for genetic heterogeneity in the Turkish population.

A N Akarsu1, U Saatci, S Ozen, A Bakkaloglu, N Besbas, M Sarfarazi.   

Abstract

Familial Mediterranean fever (FMF) is an autosomal recessive condition that is almost entirely restricted to the non-Askhenazi Jews, Arabs, Armenians, and Turks. Genetic linkage study of a large group of non-Turkish families has previously mapped the FMF locus to the 16p13.3 region and shown that this locus resides 0.305 cM distal to D16S246. Furthermore, allelic association has also been shown with D16S3070 (75%) and D16S3275 (66%). However, no genetic heterogeneity has been described for any of the three major reported groups of FMF families. Here, we describe the genetic linkage relationship of the fourth major group of Turkish families and report the first evidence for genetic heterogeneity of this condition. Two point linkage analysis and haplotype inspection of 15 DNA markers from the reported region of the FMF locus identified tight linkage in a group of six Turkish FMF families. A maximum lod score of 9.115 at theta = 0.00 was observed for D16S3024. Nine other DNA markers provided similar evidence of linkage with lod score values of above 5.21. However, two other FMF families were completely unlinked to this region of chromosome 16. Haplotype construction of DNA markers in five consanguineous linked families showed that a segment of homozygosity has been conserved for D16S3070 and D16S2617. No other DNA markers showed any such conservation. Therefore, we suggested that these two markers reside in close proximity to the FMF locus. Furthermore, we observed 80% allelic association with D16S2617 but no association with D16S3070 or any other DNA markers from the FMF critical region. In summary, we conclude that our Turkish families are also linked to the reported FMF locus at 16p13.3, there is a genetic heterogeneity for this condition at least in our group of Turkish families, and D16S2617 is in linkage disequilibrium in the Turkish FMF families. Combination of this study with previously published observations suggests that the FMF locus resides between D16S246 and D16S3070/D16S2617 and within a region of about 250-300 kb.

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Year:  1997        PMID: 9222966      PMCID: PMC1050998          DOI: 10.1136/jmg.34.7.573

Source DB:  PubMed          Journal:  J Med Genet        ISSN: 0022-2593            Impact factor:   6.318


  21 in total

1.  Localization of the familial Mediterranean fever gene (FMF) to a 250-kb interval in non-Ashkenazi Jewish founder haplotypes. The French FMF Consortium.

Authors: 
Journal:  Am J Hum Genet       Date:  1996-09       Impact factor: 11.025

2.  Familial Mediterranean Fever in Armenians. Analysis of 100 cases.

Authors:  A D Schwabe; R S Peters
Journal:  Medicine (Baltimore)       Date:  1974-11       Impact factor: 1.889

Review 3.  Familial Mediterranean fever. A survey of 470 cases and review of the literature.

Authors:  E Sohar; J Gafni; M Pras; H Heller
Journal:  Am J Med       Date:  1967-08       Impact factor: 4.965

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Authors:  A I Ozdemir; C Sokmen
Journal:  Am J Gastroenterol       Date:  1969-04       Impact factor: 10.864

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Journal:  Am J Med       Date:  1971-03       Impact factor: 4.965

6.  Familial Mediterranean fever in Armenians: autosomal recessive inheritance with high gene frequency.

Authors:  D B Rogers; M Shohat; G M Petersen; J Bickal; J Congleton; A D Schwabe; J I Rotter
Journal:  Am J Med Genet       Date:  1989-10

7.  A comprehensive genetic map of the human genome based on 5,264 microsatellites.

Authors:  C Dib; S Fauré; C Fizames; D Samson; N Drouot; A Vignal; P Millasseau; S Marc; J Hazan; E Seboun; M Lathrop; G Gyapay; J Morissette; J Weissenbach
Journal:  Nature       Date:  1996-03-14       Impact factor: 49.962

8.  The GDB Human Genome Data Base anno 1994.

Authors:  K H Fasman; A J Cuticchia; D T Kingsbury
Journal:  Nucleic Acids Res       Date:  1994-09       Impact factor: 16.971

9.  Easy calculations of lod scores and genetic risks on small computers.

Authors:  G M Lathrop; J M Lalouel
Journal:  Am J Hum Genet       Date:  1984-03       Impact factor: 11.025

10.  Location of the gene causing hyperimmunoglobulinemia D and periodic fever syndrome differs from that for familial Mediterranean fever. International Hyper-IgD Study Group.

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Journal:  Hum Genet       Date:  1994-12       Impact factor: 4.132

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  5 in total

1.  Mutation and haplotype studies of familial Mediterranean fever reveal new ancestral relationships and evidence for a high carrier frequency with reduced penetrance in the Ashkenazi Jewish population.

Authors:  I Aksentijevich; Y Torosyan; J Samuels; M Centola; E Pras; J J Chae; C Oddoux; G Wood; M P Azzaro; G Palumbo; R Giustolisi; M Pras; H Ostrer; D L Kastner
Journal:  Am J Hum Genet       Date:  1999-04       Impact factor: 11.025

2.  Exclusion of the familial Mediterranean fever locus as a susceptibility region for autosomal dominant familial Hibernian fever.

Authors:  M F McDermott; E M McDermott; K A Quane; L C Jones; B W Ogunkolade; D Curtis; F Waldron-Lynch; M Phelan; G A Hitman; M G Molloy; R J Powell
Journal:  J Med Genet       Date:  1998-05       Impact factor: 6.318

Review 3.  Familial mediterranean fever: revisiting an ancient disease.

Authors:  Seza Ozen
Journal:  Eur J Pediatr       Date:  2003-05-16       Impact factor: 3.183

4.  Variable expression of vasculitis in siblings with familial Mediterranean fever.

Authors:  Bärbel Lange-Sperandio; Klaus Möhring; Frank Gutzler; Otto Mehls
Journal:  Pediatr Nephrol       Date:  2004-03-11       Impact factor: 3.714

5.  Familial Mediterranean fever with a single MEFV mutation: where is the second hit?

Authors:  Matthew G Booty; Jae Jin Chae; Seth L Masters; Elaine F Remmers; Beverly Barham; Julie M Le; Karyl S Barron; Steve M Holland; Daniel L Kastner; Ivona Aksentijevich
Journal:  Arthritis Rheum       Date:  2009-06
  5 in total

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