HPLC法测定加替沙星注射液的含量

采用HPLC法测定加替沙星注射液含量。方法精密，准确度高，重现性好。在4.4μg/ml-21.4μg/ml浓度范围内线性关系好。回收率为99.8%，RSD为0.7%。操作简便，结果准确。     

Lack of prophylactic efficacy of an enteric-coated bovine hyperimmune milk product against enterotoxigenic Escherichia coli challenge administered during a standard meal

Orally administered bovine immunoglobulins with specific activity against colonization factors of enterotoxigenic Escherichia coli (ETEC) could provide passive protection against ETEC challenge in volunteers. Twenty healthy adult volunteers ingested either a placebo or a partially enteric-coated preparation of bovine immunoglobulins with activity against the colonization factor antigens CFA/I, CS3, and CS6 and then were challenged with ETEC strain E24377A (CS1+, CS3+) administered with a standard meal. There was no difference in the incidence or severity of diarrhea among the 10 volunteers who received the bovine immunoglobulins and the 10 who received placebo. Either the specificity or titer of anti-colonization factor antibodies or the formulation of antibodies in this product was not adequate to provide passive protection against ETEC challenge.     

Prevalence of transfusion-transmitted Chagas disease among multitransfused patients in Brazil

Background

Prevalence and risk factors for Chlamydia trachomatis infection among young men in Switzerland is still unknown. The objective of the present study was to assess prevalence and risk factors for C. trachomatis infection in young Swiss men.

Methods

517 young Swiss men were enrolled in this cross-sectional study during their compulsory military recruitment. Participants completed a questionnaire and gave urine samples which were screened for C. trachomatis DNA by PCR. Genotyping of positive samples was done by amplification and sequencing the ompA gene.

Results

The prevalence of chlamydial infection among young Swiss male was 1.2% (95% confidence interval [95%CI], 0.4–2.5%). C. trachomatis infection was only identified among the 306 men having multiple sexual partner. Although frequent, neither unprotected sex (absence of condom use), nor alcohol and drug abuse were associated with chlamydial infection. Men living in cities were more frequently infected (2.9%, 95%CI 0.8–7.4%) than men living in rural areas (0.5%, 95%CI 0.1–1.9%, p = 0.046). Moreover, naturalised Swiss citizens were more often positive (4.9%, 95%CI 1.3–12.5%) than native-born Swiss men (0.5%, 95%CI 0.1–1.7%, p = 0.003).

Conclusion

In comparison with other countries, the prevalence of chlamydial infection in men is extremely low in Switzerland, despite a significant prevalence of risky sexual behaviour. C. trachomatis infection was especially prevalent in men with multiple sexual partners. Further research is required (i) to define which subgroup of the general population should be routinely screened, and (ii) to test whether such a targeted screening strategy will be effective to reduce the prevalence of chlamydial infection among this population.     

Onset and duration of protective immunity in challenged volunteers after vaccination with live oral cholera vaccine CVD 103-HgR.

CVD 103-HgR is a live oral cholera vaccine that, in phase I and II studies to date, has been well tolerated and immunogenic. In challenge studies of US volunteers conducted 4-5 weeks after vaccination, CVD 103-HgR provided significant protection against experimental cholera due to classical and El Tor Vibrio cholerae O1. To determine the onset and duration of protection, two volunteer challenge studies were conducted: the first, 6 months after vaccination and the second, 8 days after vaccination. In both studies, CVD 103-HgR was 100% protective against diarrhea and significantly reduced the rate of shedding of vibrios after challenge with V. cholerae classical Inaba strain 569B, the virulent parent strain of CVD 103-HgR. Previously vaccinated subjects were less likely than naive controls to develop rises in titer of vibriocidal antibodies after challenge (P = .002), and the mean peak titer of vibriocidal antibodies was less than among controls. CVD 103-HgR can provide homologous protective immunity as soon as 8 days after vaccination and protection can persist for at least 6 months.     

Phase II safety and immunogenicity study of live chikungunya virus vaccine TSI-GSD-218

We conducted a phase II, randomized, double-blind, placebo-controlled, safety and immunogenicity study of a serially passaged, plaque-purified live chikungunya (CHIK) vaccine in 73 healthy adult volunteers. Fifty-nine volunteers were immunized one time subcutaneously with the CHIK vaccine and 14 were immunized with placebo (tissue culture fluid). Vaccinees were clinically evaluated intensively for one month, and had repeated blood draws for serological assays (50% plaque-reduction neutralization test) for one year. Except for transient arthralgia in five CHIK vaccinees, the number and severity of local and systemic reactions and abnormal laboratory tests after immunization were similar in CHIK vaccinees and placebo recipients. Fifty-seven (98%) of 58 evaluable CHIK vaccinees developed CHIK neutralizing antibody by day 28, and 85% of vaccinees remained seropositive at one year after immunization. No placebo recipients seroconverted. This promising live vaccine was safe, produced well-tolerated side effects, and was highly immunogenic.     

Efficacy of bovine milk immunoglobulin concentrate in preventing illness after Shigella flexneri challenge.

The protective efficacy of oral bovine immunoglobulin concentrates derived from colostrum against challenge with Shigella flexneri was studied in healthy adult volunteers in a randomized, double-blind fashion. Volunteers were given a product consisting of hyperimmune immunoglobulin concentrate with a high titer of anti-S. flexneri 2a lipopolysaccharide (LPS) with sodium bicarbonate or a control preparation with sodium bicarbonate three times a day for seven days. On the third day of treatment, volunteers received a challenge of 10(3) colony-forming units of S. flexneri 2a strain 2457T. None of the volunteers who received the high-titered hyperimmune product became ill, compared with 45% of volunteers who received the placebo (P less than 0.05). The duration of shedding of the challenge organism was decreased, and the active immune responses to S. flexneri LPS were less frequent and of lower magnitude in volunteers given the immunoglobulin concentrate than in those in the control group. High-titered, orally administered bovine immunoglobulin concentrate protects against shigellosis and may be useful in preventing shigellosis among travelers, military personnel, and individuals at risk during a Shigella outbreak.     

Low Frequency of CXCR4-Using Viruses in Patients at the Time of Primary Non-Subtype-B HIV-1 Infection

We used genotypic and phenotypic assays to estimate the frequency of X4/DM viruses in 131 patients infected with non-subtype-B viruses at the time of primary HIV-1 infection (PHI). All patients were enrolled in the French PRIMO Cohort from 1996 to 2007. Most strains belonged to CRF02_AG (51.1%) and subtype A (14.5%). Sixteen viruses (12.2%) were classified as CXCR4 tropic (“X4 strains”) by the combined criteria of amino acids 11 and 25 of the V3 loop (11/25) and net charge rules and/or the SVMgeno2pheno_10% algorithm: 6 strains by the combined genotypic rule, 7 by the SVMgeno2pheno_10% algorithm, and 3, clustering in subtype D, by both algorithms. However, only one strain (0.8%), belonging to subtype A, was defined as a dual-tropic (DM) virus by the phenotypic assay. The 67 CRF02_AG strains included 2 classified as X4 strains by the combined genotypic rule (3%) and 2 others classified as X4 strains by SVMgeno2pheno_10% (3%), but none of these 4 strains was an X4 or DM strain according to the phenotypic assay. These results suggest that the cellular virus reservoir was established with X4 strains in very few non-subtype-B-infected patients at the time of PHI. Genotypic predictions can overestimate the proportion of non-subtype-B X4 viruses at PHI.Human immunodeficiency virus type 1 (HIV-1) can be characterized by the host chemokine coreceptor that it uses to enter CD4-expressing cells. HIV-1 variants usually bind to the CCR5 chemokine coreceptor early in the course of disease. These are “R5” viruses (3, 31, 48). Viruses that use another chemokine coreceptor, CXCR4, are “X4” viruses, and they emerge later in HIV infection. They can account for up to 40 to 50% of all viruses in heavily treated patients with advanced disease (1, 32). The presence of X4 viruses has been associated with accelerated disease progression and a precipitous loss of CD4 T cells (27, 29, 40). A recent Swiss study suggested that the presence of X4 strains and the X4-specific virus load strongly predict clinical disease progression during combined antiretroviral therapy (cART), in addition to the CD4 T-cell count or viral load (44). This potential correlation between virus tropism and disease progression has important clinical implications. The development of coreceptor CCR5 antagonists for treating retroviruses and the lack of a virological response by patients infected with X4 or dual/mixed (X4/DM) viruses have increased the need to determine HIV-1 tropism.Recent studies have found the frequency of X4/DM dual-tropic strains in plasma samples from recently infected patients in the United States and Spain to be from 3.2% to 17.5% (14, 15, 16). Similarly, we found 15.9% (95% confidence interval [CI], 12.3% to 19.5%) strains of X4/DM viruses in 390 HIV-1 subtype B-infected patients diagnosed at the time of primary HIV-1 infection (PHI) in France from 1996 to 2007 (18).One of the major challenges of determining tropism is to select the best method for identifying coreceptor usage. HIV coreceptor usage is most commonly determined with a recombinant phenotype assay in clinical studies (28, 45). Bioinformatic tools based on the virus genotype may also be able to predict coreceptor usage. They are faster, less expensive, and more suitable for studies of a large number of patients than are phenotypic recombinant assays. Each available genotypic test is adequately specific but not very sensitive for detecting X4/DM or X4 variants. An overall concordance of 71.2 to 92% between genotypic and phenotypic assays has been reported (8, 15, 37, 41). However, most of these studies included HIV-1 subtype B strains. Genotypic algorithms may not be suitable for predicting the tropism of non-subtype-B HIV-1 strains (20). Two recent studies demonstrated that genotypic tests performed well for predicting the coreceptor usage of CRF02_AG and subtype C strains (36, 38), but no study has examined the correlation between genotypic and phenotypic tests for predicting the tropism of non-subtype-B HIV-1 at the time of PHI. The French PRIMO Cohort contained a large proportion of patients infected with a non-subtype-B virus (25.5% in 2005 to 2006) (6).We have therefore estimated the frequency of X4/DM viruses in 131 patients infected with non-subtype-B viruses at the time of PHI. All of them were enrolled in the French PRIMO Cohort from 1996 to 2007. We also studied the concordance between genotypic and phenotypic assays for predicting the tropism of non-subtype-B viruses in these patients.     

Virological characterization of an infection with a dual-tropic, multidrug-resistant HIV-1 and further evolution on antiretroviral therapy

We studied a case of recent infection with multidrug-resistant (MDR) HIV-1. Over 16 months off-therapy, the CD4 cell count decreased from 419 to 184 cells/mul. Antiretroviral therapy (ART) then led to an incomplete virological response but to an immunological benefit, concurrently with a shift to CCR5-only tropism and a reduction in replication capacity. ART, even if suboptimal, can be of interest in the case of MDR virus infection.