Josep M. Sierra

Blood culture flasks for culturing synovial fluid in prosthetic joint infections.

BackgroundIdentifying the etiologic microorganism is essential to guide antimicrobial therapy in prosthetic joint infection.Questions/purposeWe (1) compared the frequency of positive cultures with synovial fluid inoculated in blood culture flasks (SF) with those of periprosthetic tissues or swabs in traditional cultures from patients with acute and chronic prosthetic joint infections (PJI) and (2) determined the sensitivity, specificity, and predictive values of the three methods.Patients and MethodsWe retrospectively reviewed 87 patients with PJIs (54 knees, 33 hips) and 63 patients with aseptic loosening (34 knees, 29 hips). Two SF, periprosthetic tissue, and swab samples were taken for culture in all 150 patients except for 14 in whom only one SF fluid sample was obtained. Synovial fluid was inoculated in blood culture flasks and periprosthetic tissue and swab samples in standard media. Positive cultures were identified with standard biochemical procedures.ResultsSF samples were positive in 78 of 87 infected cases (90%), periprosthetic tissue samples were positive in 71 (82%), and swab samples were positive in 59 (68%). SF, periprosthetic tissue, and swab samples were positive more frequently in acute than in chronic infections (96% versus 82% for SF, 87% versus 74% for periprosthetic tissue, and 87% versus 44% for swabs). The sensitivity, specificity, and positive and negative predictive values of SF were 91, 100, 100, and 93 for acute infections and 79, 100, 100, and 88 for chronic infections, respectively.ConclusionsSF samples cultured in flasks had higher sensitivity, specificity, and positive and negative predictive values for diagnosis of PJI when compared with standard tissue and swab samples. The usefulness of all samples was less in chronic than in acute infections.Level of Evidence Level II, diagnostic study. See Guidelines for Authors for a complete description of levels of evidence.

Outcome of Acute Prosthetic Joint Infections Due to Gram-Negative Bacilli Treated with Open Debridement and Retention of the Prosthesis

ABSTRACT The aim of our study was to evaluate the outcome of acute prosthetic joint infections (PJIs) due to gram-negative bacilli (GNB) treated without implant removal. Patients with an acute PJI due to GNB diagnosed from 2000 to 2007 were prospectively registered. Demographics, comorbidity, type of implant, microbiology data, surgical treatment, antimicrobial therapy, and outcome were recorded. Classification and regression tree analysis, the Kaplan-Meier survival method, and the Cox regression model were applied. Forty-seven patients were included. The mean age was 70.7 years, and there were 15 hip prostheses and 32 knee prostheses. The median number of days from the time of arthroplasty was 20. The most frequent pathogens were members of the Enterobacteriaceae family in 41 cases and Pseudomonas spp. in 20 cases. Among the Enterobacteriaceae, 14 were resistant to ciprofloxacin, while all Pseudomonas aeruginosa isolates were susceptible to ciprofloxacin. The median durations of intravenous and oral antibiotic treatment were 14 and 64 days, respectively. A total of 35 (74.5%) patients were in remission after a median follow-up of 463 days (interquartile range, 344 to 704) days. By use of the Kaplan-Meier survival curve, a C-reactive protein (CRP) concentration of ≤15 mg/dl (P = 0.03) and receipt of a fluoroquinolone, when all GNB isolated were susceptible (P = 0.0009), were associated with a better outcome. By use of a Cox regression model, a CRP concentration of ≤15 mg/dl (odds ratio [OR], 3.57; 95% confidence interval [CI], 1.05 to 12.5; P = 0.043) and receipt of a fluoroquinolone (OR, 9.09; 95% CI, 1.96 to 50; P = 0.005) were independently associated with better outcomes. Open debridement without removal of the implant had a success rate of 74.5%, and the factors associated with good prognosis were a CRP concentration at the time of diagnosis ≤15 mg/dl and treatment with a fluoroquinolone.

Outcome and predictors of treatment failure in early post‐surgical prosthetic joint infections due to Staphylococcus aureus treated with debridement

Experience with debridement and prosthesis retention in early prosthetic joint infections (PJI) due to Staphylococcus aureus is scarce. The present study aimed to evaluate the outcome and predictors of failure. Patients prospectively registered with an early PJI due to S. aureus and 2 years of follow-up were reviewed. Demographics, co-morbidity, type of implant, clinical manifestations, surgical treatment, antimicrobial therapy and outcome were recorded. Remission was defined when the patient had no symptoms of infection, the prosthesis was retained and C-reactive protein (CRP) was ≤ 1 mg/dL. Univariate and multivariate analysis were performed. Fifty-three patients with a mean ± SD age of 70 ± 10.8 years were reviewed. Thirty-five infections were on knee prosthesis and 18 were on hip prosthesis. The mean ± SD duration of intravenous and oral antibiotics was 10.6 ± 6.7 and 88 ± 45.9 days, respectively. After 2 years of follow-up, 40 (75.5%) patients were in remission. Variables independently associated with failure were the need for a second debridement (OR 20.4, 95% CI 2.3-166.6, p 0.006) and a CRP > 22 mg/dL (OR 9.8, 95% CI 1.5-62.5, p 0.01). The onset of the infection within the 25 days after joint arthroplasty was at the limit of significance (OR 8.3, 95% CI 0.8-85.6, p 0.07). Debridement followed by a short period of antibiotics is a reasonable treatment option in early PJI due to S. aureus. Predictors of failure were the need for a second debridement to control the infection a CRP > 22 mg/dL and the infection onset within the first 25 days after joint arthroplasty.

Chimerism analysis following allogeneic peripheral blood stem cell transplantation with reduced-intensity conditioning.

Summary:We have performed a prospective study to evaluate early chimerism and its kinetics after allogeneic peripheral blood stem cell transplantation among 68 patients who received a reduced-intensity conditioning (RIC) regimen with fludarabine plus melphalan (n=40) or busulphan (n=28). Chimerism was analyzed by polymerase chain reaction amplification of short tandem repeats in unfractionated (UF) and/or fractionated nucleated cells from bone marrow and peripheral blood (PB). All of the patients showed initial donor engraftment and no patient presented primary or secondary graft failure. In UF samples, the probability of achieving stable complete donor chimerism (CDC) in PB within the first 6 months was 70% on day +30, 85% on day +100 and 95% on day +180. CDC in granulocytes was observed in nearly all cases from day +30 onwards. CDC in T cells, however, differed among melphalan and busulphan recipients during the first 3 months (100 vs 0% on day +30 and 93 vs 20% on day +90, respectively). In multivariate analysis, the only significant variable associated with the achievement of early CDC was having received more than two lines of chemotherapy pretransplant (P<0.02). No correlation was found between the rate of achieving early CDC and the occurrence of acute graft-versus-host disease (GVHD) or disease progression post-transplant. In multivariate analysis, the only variable that influenced the incidence of disease progression post-transplant was the development of chronic extensive GVHD (P<0.05). In conclusion, a state of CDC is readily obtained within the first 6 months after our RIC protocols. Donor myeloid engraftment occurs rapidly in all cases, while early T-cell CDC is more common in more immunosuppressed hosts and, perhaps, in melphalan recipients.

Reduced-intensity conditioning allogeneic transplantation is associated with a high incidence of extramedullary relapses in multiple myeloma patients

Reduced-intensity conditioning allogeneic transplantation is associated with a high incidence of extramedullary relapses in multiple myeloma patients

Comparable non-relapse mortality and survival after HLA-identical sibling blood stem cell transplantation with reduced or conventional-intensity preparative regimens for high-risk myelodysplasia or acute myeloid leukemia in first remission

We prospectively compared two strategies of allogeneic PBSCT from HLA-identical siblings in adults with poor-risk AML or myelodysplastic syndrome with >5% marrow blasts in an early disease status (AML or refractory anemia with excess blasts (RAEB type 2) in first remission after chemotherapy or untreated RAEB type 1). Based only on age, all consecutive patients were offered one of two specific transplant protocols. Patients ⩽50 years old received conventional high-dose conditioning with cyclophosphamide-TBI and use of CD34+-selected PBSCT (CTCD34+ group), while patients aged >50 years received a reduced-intensity conditioning (RIC) with fludarabine and oral busulphan (FB-RIC). Seventy-five patients entered the study (35 in the CTCD34+ and 39 in the FB-RIC group). The median follow-up was >4 years in both groups. The 4-year non-relapse mortality (NRM) was 19 and 20%, respectively (P=0.8). Relapse and survival were also equivalent in both groups. These results suggest that in this setting, the expected high NRM in elderly patients can be reduced with an RIC regimen.

High prevalence of nalidixic acid resistant, ciprofloxacin susceptible phenotype among clinical isolates of Escherichia coli and other Enterobacteriaceae

Therapeutic failure of infections during their treatment with quinolones has been often described. This may be due to the development of resistance during treatment of an infecting strain which already had diminished susceptibility to quinolones, even though the initial MIC did not exceed the breakpoint. In this study the prevalence of the nalidixic acid resistant, ciprofloxacin susceptible phenotype among Enterobacteriaceae was analyzed. The results showed that 113 out of 151 (74.83%) strains of the Enterobacteriaceae with diminished susceptibility to ciprofloxacin (MICs from 0.06 to 1 microg/ml) were resistant to nalidixic acid (MICs > 32 microg/ml). The Escherichia coli strains presenting this phenotype already have a mutation in the amino acid codon Ser-83 of the gyrA gene, so that the possibility of developing a second mechanism of resistance during treatment is very high.

In vitro activity of rifaximin against enteropathogens producing traveler's diarrhea

Nowadays, around 40 to 60% of Spanish travelers to developing countries develop diarrhea (4). Different enteropathogens have been associated with the development of travelers diarrhea. The levels of prevalence of these enteropathogens as a cause of travelers diarrhea are 42% for diarrheagenic Escherichia coli, 19.4% for Shigella spp., 3% for Salmonella spp., 2% for Campylobacter spp., 2% for Yersinia spp., 2% for Aeromonas spp., and <2% for others (4). Infectious diarrhea is usually a self-limited disease lasting a few days and does not require antibiotic therapy. In some cases, antimicrobial therapy is recommended (2); however, high levels of resistance to several antimicrobial agents have been described. To resolve the problem of this increase in resistance, the activities of new antimicrobial agents should be studied. Rifaximin is a nonabsorbable antibiotic (2, 5, 6) achieving concentrations of 4,000 to 8,000 μg/g in feces, with a common therapeutic dosage being 800 mg divided in two oral administrations (7). The main aim of this study was to evaluate the in vitro activity of rifaximin against enteropathogens isolated as a cause of travelers diarrhea. MICs of several antimicrobial agents for 177 enteropathogens (Table ​(Table1)1) were determined by the agar dilution method according to guidelines of the National Committee for Clinical Laboratory Standards (8). E. coli ATCC 29522 was used as a quality control strain. TABLE 1 MIC50s, MIC90s, and percentages of resistance of each antimicrobial agent for different enteropathogensa MICs at which 50 and 90% of the isolates tested were inhibited (MIC50s and MIC90s, respectively) and the percentages of resistance were calculated for each antimicrobial agent used in this study and are shown in Table ​Table11. The conventional antimicrobial agents, such as ampicillin, cotrimoxazole, tetracycline, and chloramphenicol, showed no or very little activity against the enteropathogens producing travelers diarrhea. A MIC90 of ampicillin of greater than 128 μg/ml was observed against all of the microorganisms, whereas the MIC90s of tetracycline and trimethoprim for all the microorganisms were ≥16 μg/ml. Only nalidixic acid and ciprofloxacin showed MIC90s of 256 and 32 μg/ml, respectively. The MIC90s of chloramphenicol for the different microorganisms were in a range from 8 to >128 μg/ml. Cotrimoxazole and ampicillin have been widely used to treat travelers diarrhea (3, 11, 12), and the long use and sometimes the misuse of these antibiotics have been associated with the increase of resistance levels (1, 10, 12). MIC50s and MIC90s of rifaximin and rifampin were very similar. MICs of rifaximin ranged from 4 to 8 and from 4 to 16 μg/ml, and MICs of rifampin ranged from 4 to 16 and from 8 to 16 μg/ml, for all tested bacteria except Yersinia enterocolitica and C. jejuni. In particular, the MIC50 and MIC90 of rifamixin of 64 and 128 μg/ml, respectively, were observed for Y. enterocolitica and a value of >128 μg/ml for both the MIC50 and MIC90 was achieved for C. jejuni. In this case and only for rifaximin, doses greater than 128 μg/ml were tested to determine the precise MIC50s and MIC90s, which were found to be 256 and 512 μg/ml, respectively. The in vitro activities of rifaximin against strains from stock culture collections of four university-associated teaching hospitals had been previously reported by Hoover et al. (6). In that study, the activities of rifaximin against enteropathogens were found to be as follows: a MIC50 of 4 to 8 μg/ml and a MIC90 of >8 μg/ml. These results are in accordance with ours, even though our strains were isolated from patients who traveled to different geographical areas. In another study, Ripa et al. (9) tested rifaximin against Campylobacter and Yersinia strains collected from patients with diarrhea. The main difference between these studies and ours is the MICs of rifaximin for Y. enterocolitica and C. jejuni, two microorganisms which were isolated from not more than 2% of patients with travelers diarrhea in our laboratory (3). In conclusion, rifaximin is a nonabsorbable antimicrobial agent, reaching high concentrations in the intestinal tract. The concentrations of rifaximin achieved in the intestinal tract are more than 10-fold higher than the MICs of this antimicrobial agent for the different enteropathogens used in our study. In particular, we observed a definitely good in vitro activity of rifaximin against several enteropathogens, such as E. coli, Shigella spp., and Salmonella spp., which is in accordance with clinical and microbiological outcomes of two recent studies of travelers diarrhea (2; H. L. DuPont, Z. D. Jiang, C. D. Ericsson, J. J. Mathewson, J. Aldachi, E. Palazini, L. S. Riopel, D. Ashley, and F. Martinez-Sandoval, Abstr. 39th Intersci. Conf. Antimicrob. Agents Chemother., abstr. 2227, p. 698, 1999).

MTX or mycophenolate mofetil with CsA as GVHD prophylaxis after reduced-intensity conditioning PBSCT from HLA-identical siblings

Mycophenolate mofetil (MMF) in combination with CsA seems to lead to earlier post transplant hematological recovery and less mucositis than MTX, with a similar incidence of GVHD. In this study we analyzed the post transplant outcomes of two cohorts of patients who underwent an HLA-identical sibling reduced intensity conditioning transplantation (allo-RIC) with GVHD prophylaxis consisting of CsA in combination with either MMF or a short course of MTX. We included 145 consecutive allo-RIC transplants performed between April 2000 and August 2007. The median follow-up for survivors was 41 months (4–105 months). The study group included 91 males. Median age was 55 years (range 18–71 years). Diagnoses included myeloid (n=65) and lymphoid (n=80) malignancies. GVHD prophylaxis consisted of CsA/MMF in 52 and CsA/MTX in 93 patients. The conditioning regimen was based on fludarabine in combination with BU (n=59) or melphalan (n=86). The occurrence of grade 2–4 mucositis was higher in the CsA/MTX group than in the CsA/MMF group (57 vs 23%, P=0.001). The cumulative incidence of acute and chronic GVHD was similar, 48 vs 50% and 71 vs 68%, respectively (P>0.7). The 2-year relapse and OS were similar in the CsA/MTX and CsA/MMF groups (29 vs 21%, P=0.3 and 52 vs 51%, P=0.7, respectively). Our results support further prospective studies comparing the use of the CsA/MMF combination with CsA/MTX as GVHD prophylaxis in HLA-identical sibling donor allo-RIC recipients.

Elderly age and prior autologous transplantation have a deleterious effect on survival following allogeneic peripheral blood stem cell transplantation with reduced-intensity conditioning: results from the spanish multicenter prospective trial

Summary:Over a 3-year period, 145 patients ineligible for myeloablative conditioning underwent reduced-intensity conditioning (RIC) hematopoietic stem cell transplantation (SCT) from an HLA-identical sibling in a prospective study. The median age was 54 years, 88 patients were male and 61 patients were beyond the early-intermediate phase of their disease. The 100-day probability of developing grade II–IV acute graft-versus-host disease (GVHD) was 34%, and the 1-year probability of developing chronic extensive GVHD was 41%. The 1-year probabilities of transplant-related mortality (TRM), overall (OS) and progression-free survival were 20, 60 and 52%, respectively. Multivariate analyses found a better OS in: (i) patients <60 years; and (ii) recipients of a first SCT; and a higher TRM in: (i) age >60 years, (ii) recipients of a prior autologous SCT, and (iii) an ECOG performance status >1. The 1-year TRM in patients with 0 or 1 and >2 of the above-mentioned adverse prognostic factors were 17 vs 53%, respectively (P<0.001). In summary, our study shows that elderly patients have a higher TRM following an RIC protocol. However, age by itself should not preclude these RIC transplants, since TRM appears to be unacceptably high only in the presence of additional adverse factors.