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Asociación entre el fenotipo fisura labiopalatina no sindrómica y marcadores de microsatélite ubicados en 4q / Association between nonsyndromic cleft lip/palate with microsatellite markers located in 4q
Paredes A., Mónica; Carreño Z., Hernán; Solá A., José Antonio; Segú C., Jorge; Palomino Zúñiga, Hernán; Blanco Castillo, Rafael.
Affiliation
  • Paredes A., Mónica; s.af
  • Carreño Z., Hernán; Universidad de Chile. Facultad de Medicina. ICBM. Programa de Genética Humana.
  • Solá A., José Antonio; s.af
  • Segú C., Jorge; s.af
  • Palomino Zúñiga, Hernán; Universidad de Chile. Facultad de Medicina. ICBM. Programa de Genética Humana.
  • Blanco Castillo, Rafael; Universidad de Chile. Facultad de Medicina. ICBM. Programa de Genética Humana.
Rev. méd. Chile ; 127(12): 1431-8, dic. 1999. tab
Article de Es | LILACS | ID: lil-258066
Bibliothèque responsable: CL1.1
RESUMO

Background:

Nonsyndromic cleft lip with or without cleft palate (NSCLP) is a common craniofacial defect. Association studies have suggested that a cleftinglocus is located on chromosome 4q at or near two microsatellite markers D4S175 and D4S192.

Aim:

To test the hypothesis on the possible presence of a clefting locus on chromosome 4q. Material and

methods:

We carried out an association study on a sample of unrelated NSCLP patients, of their unaffected relatives and in controls. Both probands and relatives were further analyzed depending if they originated from simplex or multiplex families. DNA was analyzed with two PCR markers close to the putative NSCLP locus, dinucleotide repeats D4S175 and D4S192. PCR products were resolved by PAGE and visualized by silver staining. Statistical analysis was performed by means of c2 log ratio.

Results:

Significant differences between NSCLP and controls were observed when comparing the allele frequency distribution of D4S192 both in the total sample as well as in NSCLP-multiplex and simplex cases. No significant differences for D4S175 were observed in any of the comparisons. Unaffected relatives showed significant differences with controls both for D4S175 and D4S192.

Conclusions:

Our results support the hypothesis that a NSCLP locus maps on chromosome 4q close to the microsatellite marker D4S192. No differences were observed between NSCLP multiplex and simplex cases versus controls, implying that they do not represent different etiologic entities. The results of the present and previous studies in the same group of patients support the hypothesis that several major interacting genes participate in the etiology of NSCLP
Sujet(s)
Texte intégral: 1 Indice: LILACS Sujet Principal: Bec-de-lièvre / Fente palatine / Répétitions microsatellites Type d'étude: Observational_studies / Risk_factors_studies Limites du sujet: Adult / Female / Humans / Male langue: Es Texte intégral: Rev. méd. Chile Thème du journal: MEDICINA Année: 1999 Type: Article
Texte intégral: 1 Indice: LILACS Sujet Principal: Bec-de-lièvre / Fente palatine / Répétitions microsatellites Type d'étude: Observational_studies / Risk_factors_studies Limites du sujet: Adult / Female / Humans / Male langue: Es Texte intégral: Rev. méd. Chile Thème du journal: MEDICINA Année: 1999 Type: Article