ABSTRACT
OBJECTIVE: To compare the progression of periodontal destruction in people with and without HIV. METHOD: Relative attachment loss on 6 index teeth was compared between 19 people with HIV and 17 people without HIV infection over 12 and 18 month follow ups. RESULTS: The proportions of sites with 1, 2 or 3 mm of relative attachment loss were similar in the study and control groups. Mean maximum relative attachment loss was similar in both groups after 12 months but greater in the study group after 18 months. CONCLUSIONS: The data are not compelling evidence of greater periodontal destruction associated with HIV infection. Large scale cohort studies or meta-analyses would be more conclusive.
Subject(s)
HIV Infections/complications , Periodontal Attachment Loss/classification , Adult , CD4 Lymphocyte Count , Case-Control Studies , Chi-Square Distribution , Dental Plaque/classification , Disease Progression , Female , Follow-Up Studies , Humans , Longitudinal Studies , MaleABSTRACT
The WHO Alliance for Global Elimination of Trachoma by 2020 has increased the need to identify ocular chlamydial infections by clinical examination in areas of both high and low prevalence. The relationship between clinically active trachoma (as defined by clinical examination) and chlamydial infection is known for areas with hyperendemic trachoma, but not for areas with a low prevalence of the clinical disease. In the present study, we examined, photographed, and DNA tested the conjunctivae of children in the Surkhet district of mid-western Nepal, an area known to have a low prevalence of clinically active trachoma. Although 6% of the children aged 10 years and under were found to have clinically active trachoma, none were found to have chlamydia infection by the most sensitive DNA amplification tests available. A very low prevalence of clinically active trachoma is not necessarily evidence of the presence of chlamydial infection. Therefore, the WHO policy of not recommending an intensive trachoma control effort when the prevalence of clinically active trachoma is less than 10% in children is appropriate for this area of Nepal.
PIP: This article assesses the reliability of clinical diagnosis in identifying trachoma in a low prevalence area in Nepal. WHO¿s Alliance for Global Elimination of Trachoma by the year 2020 depends on the identification of communities in which blinding trachoma is present and of individuals in these communities who are seeking treatment. All children aged 1-10 from 6 villages in the Surkhet district of the Bheri zone underwent clinical tests, which were administered between November 17 and December 1, 1997. 726 out of 765 children were examined. 125 among these were further evaluated by photography and DNA testing on their right conjunctivae. Clinically active disease was found in 46 out of 726 children seen by the first examiner. Photographic evaluation showed that 32 of these 46 children had clinically active disease, while 14 of 79 children were found negative of the disease on examination. The results revealed that there was a low prevalence of active conjunctival disease in this area: only 6% of the children were clinically active on examination, and none were found to have chlamydia infection as assessed by the most sensitive DNA amplification test available. The WHO policy of not recommending an intensive trachoma control effort when the prevalence of clinically active trachoma is less than 10% in children is therefore appropriate for this area in Nepal. Clinical examination is the only feasible way of estimating the prevalence of infection; however, very low prevalence of active trachoma is not evidence for the presence of chlamydial infection.
Subject(s)
Trachoma/diagnosis , Child , Child, Preschool , Female , Humans , Infant , Male , Nepal/epidemiology , Predictive Value of Tests , Prevalence , Rural Population , Sensitivity and Specificity , Trachoma/epidemiologySubject(s)
Trachoma , Predictive Value of Tests , Reproducibility of Results , Cross-Sectional Studies , NepalABSTRACT
The financial viability of programme services and product offerings requires that revenue exceeds expenses. Revenue includes payments for services and products as well as donor cash and in-kind contributions. Expenses reflect consumption of purchased or contributed time and materials and utilization (depreciation) of physical plant facilities and equipment. Standard financial reports contain this revenue and expense information, complemented when necessary by valuation and accounting of in-kind contributions. Since financial statements are prepared using consistent and accepted accounting practices, year-to-year and organization-to-organization comparisons can be made. The use of such financial information is illustrated in this article by determining the unit cost of cataract surgery in two hospitals in Nepal. The proportion of unit cost attributed to personnel, medical supplies, administrative materials, and depreciation varied significantly by institution. These variations are accounted for by examining differences in operational structure and capacity utilization.
Subject(s)
Accounting , Cataract Extraction/economics , Financial Management, Hospital , Costs and Cost Analysis , Humans , Income , Investments , NepalABSTRACT
The extent of nucleotide sequence microheterogeneity varies among subgenomic regions of Epstein-Barr virus (EBV). We examined, in EBV-carrying lymphoid cell lines, the extent of polymorphism in EBV DNA fragments amplified from the BamHI E, K, N and Z regions, and then investigated the diversity of the more hypervariable regions in tissues and body fluids. In cell lines, sequence dissimilarities in a genotype-specifying fragment of the EBNA-3C gene varied from < 1-4% within each genotype; dissimilarities in the first intron of the BZLF- 1 gene were < 2% within each genotype. By contrast, dissimilarities in a C-terminal unique domain of the EBNA-1 gene, and in a fragment that encompasses and is upstream of the LMP-1 start codon, varied between 2 and 7% and were not genotype-specific. The sequence diversity in BamHI K and N regions was then examined in tissues and body fluids by single-strand conformation polymorphism (SSCP) analysis and cycle sequencing. Extensive inter-host diversity was observed, whether the host was co-infected by human immunodeficiency virus (HIV) or not. In the oral cavity of HIV-infected patients, inter-compartmental EBV diversity could be demonstrated, even between sites that were anatomically proximate. Studies of BamHI K clones derived from EBV in oral lesions revealed infection by multiple variants. Identification of hypermutable loci within the EBV genome such as those located in the BamHI K and N regions should permit fine discrimination of individual EBV variants.
Subject(s)
Genetic Variation , Genome, Viral , Herpesvirus 4, Human/genetics , Amino Acid Sequence , Base Sequence , DNA, Viral/genetics , Humans , Molecular Sequence Data , Polymorphism, Genetic , Sequence Analysis, DNAABSTRACT
OBJECTIVE: To examine risk factors associated with Epstein-Barr virus (EBV) replication in the oral epithelium of an HIV-infected cohort. DESIGN: Longitudinal study of behavioural, medication and immunological parameters of HIV-1-seropositive outpatients attending a genitourinary clinic. Outcome measure was EBV DNA positivity in curetted oral squames, as detected by in situ hybridization. Logistic regression for repeated observations of the same individuals was used to analyse how risk changed over time. RESULTS: Fifty six individuals were studied; 158 patient-visits were made in total (mean, 2.8). Of 137 samples curetted from the tongue, 36 were positive for EBV DNA. Recreational drug use, oral sexual practices, therapy with zidovudine and aciclovir, and changes in CD4 and total lymphocyte counts were not associated with changes in risk. Alcohol drinking, elevated CD8 lymphocyte counts and fluconazole therapy were associated with a decreased risk, and cigarette smoking with increased risk. CONCLUSION: Behavioural and HIV-specific immunological changes may play important roles in promoting and affecting the course of oral EBV replication. Rigorous anticandidal therapy and avoidance of cigarette smoking may retard the development of oral hairy leukoplakia.
