Peritubular Capillaries C4d Deposits in Renal Allograft Biopsies and Anti HLA I/II Alloantibodies Screening. Incidence and Clinical Importance

Aim: To characterise clinically the patients with C4d in peritubular capillaries deposits (C4dPTCD) and/or circulating anti-HLA class I/II alloantibodies. To determine the correlation between positive C4dPTCD and circulating anti-HLA class I/II alloantibodies during episodes of graft dysfunction. Subjects and Methods: C4d staining was performed in biopsies with available frozen tissue obtained between January 2004 and December 2006. The study was prospective from March 2005, when a serum sample was obtained at the time of biopsy to detect circulating anti-HLA class I/II alloantibodies. Results: We studied 109 biopsies in 86 cadaver renal transplant patients. Sixteen of these (14.7%) presented diffuse positive C4dPTCD. There was a 13.5% rate of +C4dPTCD incidence within the first six months of transplantation and 16% after six months (p>0.05). Half of the +C4dPTCD in the first six months was associated with acute humoral rejection. After six months, the majority of +C4dPTCD (n=7/8) was present in biopsies with evidence of interstitial fibrosis/tubular atrophy and/or transplant glomerulopathy. The C4dPTCD was more frequent in patients with positive anti-HCV antibodies(p<0.0001), a previous renal transplant (p=0.007), and with a panel reactivity antibody (PRA) ≥ 50%(p=0.0098). The anti-HCV+ patients had longer time on dialysis (p=0.0019) and higher PRA(p=0.005). Circulating anti-HLA I/II alloantibodies were screened in 46 serum samples. They were positive in 10.9% of samples, all obtained after six months post transplant. Circulating alloantibodies were absent in 92.5% of the C4d negative biopsies. Conclusion: We found an association between the presence of C4dPTCD and 2nd transplant recipients,higher PRA and the presence of anti-HCV antibodies. The presence of HCV antibodies is not a risk factor for C4dPTCD per se, but appears to reflect longer time on dialysis and presensitisation. In renal dysfunction a negative alloantibody screening is associated with a reduced risk of C4dPTCD (<10%).

Hidrossalpinge e Outras Causas de Factor Tubário Efeito Deletério do Hidrossalpinge?

Introdução: A Técnica de fertilização in vitro-transferência embrionária (FIV-TE) foi desenvolvida para permitir a gravidez em mulheres com patologia tubária. Inúmeros artigos foram publicados referindo que no grupo de Infertilidade Feminina por Factor Tubário isolado (FTi), o sub-grupo de Hidrossalpinge (HS), apresentava piores resultados nos ciclos FIV-TE. Material e Métodos: Estudo retrospectivo de 99 ciclos FIV-TE efectuados em 88 mulheres com FTi entre Janeiro de 1997 e Dezembro de 1999, na Unidade de Medicina da Reprodução da Maternidade Dr. Alfredo da Costa (MAC). O objectivo foi comparar as diferentes taxas de gravidez entre o subgrupo de Hidrossalpinge (n=28) e o grupo de FTi sem hidrossalpinge (n=71). Resultados: A análise estatística entre o grupo HS e o grupo de Fti sem HS relativamente aos parâmetros do protocolo FIV foi estatisticamente não significativa. Discussão: Um grande número de estudos na literatura confirmam o efeito negativo do HS nos resultados da técnica FIV-TE, relativamente às outras causas de factor tubário, excepto os estudos de Sharara et al (1996) e Bazar et al (1995). Provavelmente as diferentes técnicas para o diagnóstico do HS resultam em diferentes percentagens de diagnóstico da patologia, interferindo nos resultados finais. Conclusão: Na população em estudo na MAC o efeito deletério do HS não demonstrou significado estatístico. No entanto, em valor absoluto a taxa de gravidez é discretamente inferior.

Differences in Nevirapine Biotransformation as a Factor for its Sex-Dependent Dimorphic Profile of Adverse Drug Reactions

OBJECTIVES: Nevirapine is widely used for the treatment of HIV-1 infection; however, its chronic use has been associated with severe liver and skin toxicity. Women are at increased risk for these toxic events, but the reasons for the sex-related differences are unclear. Disparities in the biotransformation of nevirapine and the generation of toxic metabolites between men and women might be the underlying cause. The present work aimed to explore sex differences in nevirapine biotransformation as a potential factor in nevirapine-induced toxicity. METHODS: All included subjects were adults who had been receiving 400 mg of nevirapine once daily for at least 1 month. Blood samples were collected and the levels of nevirapine and its phase I metabolites were quantified by HPLC. Anthropometric and clinical data, and nevirapine metabolite profiles, were assessed for sex-related differences. RESULTS: A total of 52 patients were included (63% were men). Body weight was lower in women (P = 0.028) and female sex was associated with higher alkaline phosphatase (P = 0.036) and lactate dehydrogenase (P = 0.037) levels. The plasma concentrations of nevirapine (P = 0.030) and the metabolite 3-hydroxy-nevirapine (P = 0.035), as well as the proportions of the metabolites 12-hydroxy-nevirapine (P = 0.037) and 3-hydroxy-nevirapine (P = 0.001), were higher in women, when adjusted for body weight. CONCLUSIONS: There was a sex-dependent variation in nevirapine biotransformation, particularly in the generation of the 12-hydroxy-nevirapine and 3-hydroxy-nevirapine metabolites. These data are consistent with the sex-dependent formation of toxic reactive metabolites, which may contribute to the sex-dependent dimorphic profile of nevirapine toxicity.