Hereditary deficiency of the seventh component of complement and recurrent meningococcal infection: investigations of an Irish family using a novel haemolytic screening assay for complement activity and C7 M/N allotyping

Egan, Laurence J.; Orren, Ann; Doherty, John D.H.; Würzner, Reinhard; McCarthy, C. F.

doi:10.1017/s0950268800051700

Cited by 12 publications

(7 citation statements)

References 19 publications

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“…In family A, subjects II.1 and II.4, both C7 deficient, have not to date developed meningococcal infection, highlighting that deficiency is not incompatible with apparently normal health [5]. Diagnosis of underlying deficiency in patients presenting with meningococcal infections does allow appropriate precautions to be taken to minimize the risk of further infections [25]. DNA polymorphisms can be detected irrespective of whether the sequence change affects the phenotype, and prior knowledge of the molecular defect responsible for the deficiency is not required.…”

Section: Discussionmentioning

confidence: 99%

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C7 deficiency in an Irish family: a deletion defect which is predominant in the Irish

O'Hara

Fernie

Moran

et al. 1998

Clinical and Experimental Immunology

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Human deficiencies of terminal complement components are known to be associated with increased susceptibility to Neisseria meningitidis infection. Polymorphic DNA marker studies in complement deficient investigations allow identification of haplotypes associated with the deficiency and enable the possible identification of heterozygote carriers of the defect. We report studies of an Irish family in which the index case had suffered recurrent meningococcal disease and was found to be deficient in the seventh component of complement (C7). The availability of all family members enabled us to determine the segregating haplotypes. The defects in the family segregated with two very closely related C6 and C7 DNA haplotypes, one of which is known to be associated with the large Irish C7 DNA deletion defect. The index case and two C7 deficient siblings were found to be homozygous for this defect, a deletion that spans approx. 6.8 kbp and encompasses exons 7 and 8. The deletion defect of exons 7 and 8 of C7 has been found in homozygous form in another C7 deficient Irish individual, and is present in heterozygous form in C7 deficient members of a third Irish family. Therefore, this deletion defect occurs in five of the six deficient chromosomes of these three unrelated Irish families, raising the interesting question of how prevalent this defect may be within the Irish community.

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Section: Discussionmentioning

confidence: 99%

“…Total functional complement activity and C7 functional activity in the serum of members of family A were tested by haemolytic assays and double diffusion haemolytic assays in 1% agarose gels [6,25].…”

Section: Functional Assaysmentioning

confidence: 99%

C7 deficiency in an Irish family: a deletion defect which is predominant in the Irish

O'Hara

Fernie

Moran

et al. 1998

Clinical and Experimental Immunology

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“…Deficiencies of terminal complement components (TCC), particularly of C5, C6, C7, and C8, are often detected because of increased susceptibility to Neisserial infections [Ross and Densen, 1984]. Much of the literature is comprised of surveys in various communities of patients with meningococcal infections who were subsequently tested for terminal component deficiencies [Eng, 1980; Ellison et al, 1983; Merino et al, 1983; Beatty et al, 1986; Leggiadro and Winklestein, 1987; Orren et al, 1987; Rasmussen et al, 1987, 1988; Zimran et al, 1987; Brai et al, 1989; Rogde et al, 1990; Schlesinger et al, 1990; Platonov et al, 1993; Egan et al, 1994]. Of interest is the nonuniform association between any specific geographic/ethnic group and meningococcal diseases.…”

Section: Introductionmentioning

confidence: 99%

C7 complement deficiency in an Israeli Arab village

et al. 2002

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Deficiencies of terminal complement components, particularly the latter ones, are often detected because of increased susceptibility to Neisserial infections. Herein we document the first report of C7 deficiency among a highly inbred Arab population living in the lower Galilee region of Israel. Both biochemical and molecular analysis were performed on samples from infected survivors and parents of children who succumbed to Neisserial infections in a 4-year period. Only the index case who suffered recurrent infections and a sibling who had not suffered an infection during the outbreak were found to be C7-deficient. The mutation was found to be the one previously described to be prevalent among Israeli Jews of Moroccan ancestry (mutation G1135C). The implications of this finding are discussed in the context of family pedigree, the protective effect of complement deficiency, and the clinical outcome.

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“…C7 is a component of the complement system. People with down-regulated C7 are prone to recurrent bacterial infections (22). As with other chemokines, the protein encoded by CCL21 inhibits hemopoiesis, and stimulates chemotaxis.…”

Section: Discussionmentioning

confidence: 99%

Expression Profiling of the Cellular Processes in Uterine Leiomyomas: Omic Approaches and IGF-2 Association with Leiomyosarcomas

et al. 2004

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Potentially significant pathogenetic cellular processes showed that down-regulated functional profiling has an important impact on the discovery of the pathogenic pathways in leiomyomas and leiomyosarcomas. GO analysis can also overcome the complexity of the expression profiles of cDNA microarrays and 2D protein analyses, via a cellular process level approach. Thereby, a valuable prognostic candidate gene, with real relevance to disease-specific pathogenesis, can be found at cellular process levels.

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Hereditary deficiency of the seventh component of complement and recurrent meningococcal infection: investigations of an Irish family using a novel haemolytic screening assay for complement activity and C7 M/N allotyping

Cited by 12 publications

References 19 publications

C7 deficiency in an Irish family: a deletion defect which is predominant in the Irish

C7 deficiency in an Irish family: a deletion defect which is predominant in the Irish

C7 complement deficiency in an Israeli Arab village

Expression Profiling of the Cellular Processes in Uterine Leiomyomas: Omic Approaches and IGF-2 Association with Leiomyosarcomas

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