Skipping of exon 27 in C3 gene compromises TED domain and results in complete human C3 deficiency.

Primary deficiency of complement C3 is rare and usually associated with increased susceptibility to bacterial infections. In this work, we investigated the molecular basis of complete C3 deficiency in a Brazilian 9-year old female patient with a family history of consanguinity. Hemolytic assays revealed complete lack of complement-mediated hemolytic activity in the patient's serum. While levels of the complement regulatory proteins Factor I, Factor H and Factor B were normal in the patient's and family members' sera, complement C3 levels were undetectable in the patient's serum and were reduced by at least 50% in the sera of the patient's parents and brother. Additionally, no C3 could be observed in the patient's plasma and cell culture supernatants by Western blot. We also observed that patient's skin fibroblasts stimulated with Escherichia coli LPS were unable to secrete C3, which might be accumulated within the cells before being intracellularly degraded. Sequencing analysis of the patient's C3 cDNA revealed a genetic mutation responsible for the complete skipping of exon 27, resulting in the loss of 99 nucleotides (3450-3549) located in the TED domain. Sequencing of the intronic region between the exons 26 and 27 of the C3 gene (nucleotides 6690313-6690961) showed a nucleotide exchange (T→C) at position 6690626 located in a splicing donor site, resulting in the complete skipping of exon 27 in the C3 mRNA.

[Conjunctivitis due to Achromobacter xylosoxidans: case report]. / Conjuntivite por Achromobacter xylosoxidans: relato de caso.

We report here a case of conjunctivitis in an immunocompetent patient due to Achromobacter xylosoxidans, which was associated with the use of rigid contact lenses. The bacteria were isolated from the scraped conjunctival swab as well as from the lens cleaning fluid. A. xylosoxidans is an opportunistic pathogen, especially in immunocompromised patients; however, in isolates of ocular infections, from immunocompetent patients, it may be confused with other gram-negative organisms, particularly Pseudomonas aeruginosa. Due to an increased resistance against different antimicrobial agents, A. xylosoxidans must be fully identified and differentiated from other gram-negative isolates from ocular infections.

Conjuntivite por Achromobacter xylosoxidans: relato de caso / Conjunctivitis due to Achromobacter xylosoxidans: case report

Relatamos um caso de conjuntivite ocasionada por Achromobacter xylosoxidans em paciente imunocompetente usuária de lentes de contato rígidas. A bactéria foi isolada da solução utilizada para a desinfecção das lentes bem como do raspado conjuntival. A. xylosoxidans tem sido descrita em infecções oportunistas em pacientes imunodeprimidos, contudo pode ser confundida com outros bacilos gram-negativos, principalmente Pseudomonas aeruginosa, isoladas de infecções oculares em pacientes imunocompetentes. Devido ao reduzido perfil de sensibilidade aos antimicrobianos demonstrado pelo A. xylosoxidans, torna-se importante a identificação deste agente etiológico em quadros de conjuntivite.

We report here a case of conjunctivitis in an immunocompetent patient due to Achromobacter xylosoxidans, which was associated with the use of rigid contact lenses. The bacteria were isolated from the scraped conjunctival swab as well as from the lens cleaning fluid. A. xylosoxidans is an opportunistic pathogen, especially in immunocompromised patients; however, in isolates of ocular infections, from immunocompetent patients, it may be confused with other gram-negative organisms, particularly Pseudomonas aeruginosa. Due to an increased resistance against different antimicrobial agents, A. xylosoxidans must be fully identified and differentiated from other gram-negative isolates from ocular infections.

Influência genética sobre a doença de Alzheimer de início precoce / Genetic influence on early onset Alzeimer's disease

CONTEXTO: A doença de Alzheimer de início precoce (DAIP) representa 5 por cento de todos os casos de doença de Alzheimer e está relacionada a mutações gênicas. OBJETIVO: Apresentar a influência de mutações gênicas na DAIP. MÉTODOS: Revisão da literatura, a partir de 1992, empregando o banco de dados PubMed. RESULTADOS: O alelo E*4 do gene da apolipoproteína E interfere na DAIP. No gene da proteína precursora da amiloide, foram descritas 20 mutações, que causam cerca de 10 por cento a 15 por cento dos casos de DAIP. Mutações no gene das presenilinas 1 e 2 causam 30 por cento a 70 por cento dos casos de DAIP. No gene da PSN1, há 30 mutações de troca de aminoácidos e três inserções/deleções. O gene da PSEN2 apresenta seis mutações de troca de aminácidos. No gene MAPT, apenas uma mutação se relaciona exclusivamente com a DA. CONCLUSÕES: O uso de informações genéticas para a detecção precoce de possíveis pacientes com DAIP ainda é bastante limitado. A heterogeneidade genética é ampla. Algumas mutações descritas nesta revisão foram responsáveis pela doença de Alzheimer em apenas algumas poucas famílias. A aplicação clínica desses métodos no rastreamento de indivíduos em risco para a DAIP ainda exige cautela.

BACKGROUND: Early onset Alzheimer's disease (EOAD) represents 5 percent of all cases of Alzheimer's disease, and it is connected to genic mutations. OBJECTIVES: To present the influence of genic mutations in EOAD. METHODS: Review of current literature, starting from 1992, utilizing the PubMed data bank. RESULTS: The E*4 allele of the apolipoprotein E gene interferes in EOAD. In the gene of the Amyloid Precursor Protein, 20 mutations were described, causing 10 percent to 15 percent of the cases of EOAD. Mutations in the gene of presenilins 1 and 2 cause 30 percent to 70 percent of the cases of EOAD. In PSN1 gene, 30 aminoacid change mutations and 3 insertions/deletions are known. In the PSEN2 gene, there are 6 aminoacid change mutations. Only one mutation in the MAPT gene is selectively associated with Alzheimer's disease. CONCLUSIONS: The use of genetic information for early detection of possible pacients of EOAD is still very limited. Genetic heterogeneity is broad. Some mutations described in this review were responsible for Alzheimer's disease only in a few families. The clinical utilization of these methods for screening individuals at risk for EOAD still asks for caution.

Influência genética sobre a doença de Alzheimer de início tardio / Genetic influence on late onset Alzeimer's disease

CONTEXTO: A doença de Alzheimer de início tardio (DAIT) representa a maior parte dos casos de doença de Alzheimer (DA). OBJETIVO: Revisar resultados relevantes para genes candidatos e de suscetibilidade para a DAIT. MÉTODOS: Revisão bibliográfica, a partir de 1990, empregando os bancos de dados PubMed e SciELO. RESULTADOS: Polimorfismos genéticos são mais relevantes para a DAIT que mutações, sendo que o alelo E*4 do gene APOE é o maior fator de risco conhecido até o momento. No entanto, outros genes vêm sendo investigados e existem dados disponíveis sobre a relação com DAIT para os genes da apolipoproteína CI, alfa-1-antiquimiotripsina, receptor sigma tipo 1, enzima conversora de angiotensina, alfa 2-macroglobulina, proteína relacionada ao receptor de LDL, interleucina 1 alfa e beta, paraoxonase, transportador de serotonina e receptores de serotonina. CONCLUSÕES: A DAIT tem etiologia multifatorial e um grande número de marcadores genéticos influencia em seu desenvolvimento. Essas variantes precisam ser investigadas na população brasileira, cuja formação étnica é distinta daquela de populações norte-americanas e europeias. Somente assim será possível a determinação do perfil genético de risco, que facilitará a detecção de indivíduos com maior probabilidade de desenvolver a doença.

BACKGROUND: Late Onset Alzheimer's disease (LOAD) represents the majority of cases of Alzheimer's disease. OBJECTIVES: To review relevant results to candidate and susceptibility genes related to LOAD. METHODS: Bibliographic review, starting from 1990, utilizing PubMed and SciELO data banks. RESULTS: Genetic polymorphisms are more relevant for LOAD than mutations, and E*4 allele of APOE gene is the major risk factor known until now. Neverthless, other genes are being investigated and data are available about the relation with LOAD to the genes coding for apolipoprotein CI, antichymotrypsin, sigma receptor type 1, angiotensin converting enzyme, alfa 2-macroglobulin, LDL receptor related protein, interleucin 1 alfa and beta, paraoxonase, serotonin transporter and serotonin receptors. CONCLUSIONS: LOAD presents multifactorial etiology, and a broad number of genetic markers interferes with its development. They should be further pursued in the Brazilian population, in which ethnic background is distinct from North-american and European populations. Only with this data, a determination of the genetic risk profile will be feasible, and will improve the detection of the individuals at greater probability of developing the disease.