{"id":26991,"date":"2015-10-26T13:24:41","date_gmt":"2015-10-26T13:24:41","guid":{"rendered":"http:\/\/healthmedicinet.com\/news\/recurrent-skin-and-soft-tissue-infections-in-hiv-infected-patients-during-a-5-year-period-incidence-and-risk-factors-in-a-retrospective-cohort-study\/"},"modified":"2015-10-26T13:24:41","modified_gmt":"2015-10-26T13:24:41","slug":"recurrent-skin-and-soft-tissue-infections-in-hiv-infected-patients-during-a-5-year-period-incidence-and-risk-factors-in-a-retrospective-cohort-study","status":"publish","type":"post","link":"http:\/\/healthmedicinet.com\/news\/recurrent-skin-and-soft-tissue-infections-in-hiv-infected-patients-during-a-5-year-period-incidence-and-risk-factors-in-a-retrospective-cohort-study\/","title":{"rendered":"Recurrent skin and soft tissue infections in HIV-infected patients during a 5-year period: incidence and risk factors in a retrospective cohort study"},"content":{"rendered":"<h4>Population characteristics<\/h4>\n<p>Of the 511 subjects in the initial cohort, 87 individuals (17.0\u00c2\u00a0%) experienced at<br \/>\n         least one SSTI, as described elsewhere 6]. Two subjects from the cohort had no follow-up time after the initial SSTI, so 85<br \/>\n         subjects were included in the analysis reported in this study. The demographics of<br \/>\n         this cohort are shown in Table\u00c2\u00a01. The 85 subjects contributed 118.3 person-years of follow-up, with subjects censored<br \/>\n         at loss to follow-up or at the time of recurrent SSTI.<\/p>\n<p><strong>Table 1.<\/strong> Baseline characteristics of individuals who did and did not develop a recurrent SSTI<br \/>\n         during the study period\n      <\/p>\n<p>Of the initial SSTIs, 50 (58.8\u00c2\u00a0%) were abscesses, 27 (31.8\u00c2\u00a0%) were furuncles, and<br \/>\n         8 (9.4\u00c2\u00a0%) were cellulitides. Incision and drainage of the initial SSTI was performed<br \/>\n         in 28 cases (32.9\u00c2\u00a0%). Only 23\/85 initial SSTIs were associated with culture data,<br \/>\n         one of which was culture-negative. <em>S. aureus<\/em> was an identified pathogen in 15 initial SSTIs, and MRSA in 11 of these. <em>Pseudomonas aeruginosa<\/em> was the only other pathogen identified in more than one patient, having been identified<br \/>\n         in 3 SSTIs. All cultures were from an infected skin site.\n      <\/p>\n<p>Of the 85 initial SSTIs, 20 (23.5\u00c2\u00a0%) were treated with combination antimicrobial drug<br \/>\n         therapy. The most common combination used was ciprofloxacin and clindamycin, used<br \/>\n         in 3 patients (3.5\u00c2\u00a0% of all patients, 15\u00c2\u00a0% of patients receiving combination therapy).<br \/>\n         Of the 65 who did not receive combination antimicrobial drug therapy, 20 (23.5\u00c2\u00a0% of<br \/>\n         all initial SSTIs) received a beta-lactam, 21 (24.7\u00c2\u00a0%) received clindamycin, 8 (9.4\u00c2\u00a0%)<br \/>\n         received trimethoprim-sulfamethoxazole, 5 (5.9\u00c2\u00a0%) received a fluoroquinolone, 2 (2.4\u00c2\u00a0%)<br \/>\n         received vancomycin, and 3 (3.5\u00c2\u00a0%) received no antimicrobial drug therapy. Whether<br \/>\n         or not antimicrobial drug therapy was prescribed for the initial SSTI was not documented<br \/>\n         in the medical records of six (7.1\u00c2\u00a0%) patients. As documented in the medical record,<br \/>\n         no subject underwent attempts at decolonization after the initial SSTI.\n      <\/p>\n<p>A total of 30 subjects among the 85 who had follow-up (35.3\u00c2\u00a0%) experienced at least<br \/>\n         one recurrent SSTI during follow-up. Using Kaplan-Meier methods, the estimated proportion<br \/>\n         of individuals who would have experienced a recurrent SSTI if all individuals had<br \/>\n         been followed for one year was 29.2\u00c2\u00a0% (95\u00c2\u00a0% CI 20.3\u00c2\u00a0%-41.0\u00c2\u00a0%), while the 3-year risk<br \/>\n         was 47.0\u00c2\u00a0% (95\u00c2\u00a0% CI 34.4\u00c2\u00a0%-61.6\u00c2\u00a0%). Figure\u00c2\u00a01 shows the estimated Kaplan-Meier cumulative incidence of SSTIs over time. The incidence<br \/>\n         of second SSTI was 253.6 SSTIs\/1000 person-years (95\u00c2\u00a0% CI 166.8-385.7). Fourteen subjects<br \/>\n         experienced multiple recurrences (16.5\u00c2\u00a0% of all subjects with initial SSTI; 46.7\u00c2\u00a0%<br \/>\n         of subjects with at least one recurrence).<\/p>\n<p><strong>Fig. 1.<\/strong> Kaplan-Meier curve demonstrating the cumulative risk of recurrent SSTI over time with<br \/>\n         95\u00c2\u00a0% confidence intervals\n      <\/p>\n<p>A number of variables assessed as potential risk factors for SSTIs were time-varying.<br \/>\n         These variables were therefore not assumed to be present throughout the follow-up<br \/>\n         period; instead, they were calculated as present or absent on each day of follow-up.<br \/>\n         For example, 79.8\u00c2\u00a0% of follow-up time accrued to individuals on Medicaid, 1.6\u00c2\u00a0% to<br \/>\n         individuals with a catheter, 24.7\u00c2\u00a0% to individuals taking trimethoprim-sulfamethoxazole<br \/>\n         prophylaxis, and 12.0\u00c2\u00a0% to individuals taking azithromycin prophylaxis. Highly active<br \/>\n         antiretroviral therapy (HAART) was being given 77.1\u00c2\u00a0% of the time, and the cohort<br \/>\n         had an HIV VL??1000 copies\/mL on 60.0\u00c2\u00a0% of days. The diagnosis of certain comorbid<br \/>\n         conditions was assessed similarly, with 14.6\u00c2\u00a0% of follow-up time occurring in subjects<br \/>\n         with diabetes, and 7.8\u00c2\u00a0% with cancer (Table\u00c2\u00a02).<\/p>\n<p><strong>Table 2.<\/strong> Proportion of patient-days with exposure to time-varying covariates\n      <\/p>\n<h4>Characteristics of recurrent SSTIs<\/h4>\n<p>The median recurrent SSTI occurred at 144\u00c2\u00a0days after the initial SSTI (interquartile<br \/>\n         range [IQR], 89\u00e2\u20ac\u201c377). Trimethoprim-sulfamethoxazole prophylaxis was being taken by<br \/>\n         5\/30 subjects (16.7\u00c2\u00a0%) at the time of SSTI, and 3\/6 (50\u00c2\u00a0%) individuals with CD4+ count??200<br \/>\n         cells\/mm<br \/><sup>3<\/sup><br \/>\n         at the time of SSTI were taking trimethoprim-sulfamethoxazole. The median CD4+ count<br \/>\n         at the time of recurrent SSTI was 403.5 (IQR 239\u00e2\u20ac\u201c529), and the median VL was 1475<br \/>\n         copies\/mL (IQR undetectable-27800). We found that 26\/30 (86.7\u00c2\u00a0%) SSTI recurrences<br \/>\n         occurred in patients with CD4+ count??100 cells\/mm<br \/><sup>3<\/sup><br \/>\n         . Of the recurrent infections, 17 were abscesses (56.7\u00c2\u00a0%), 9 were cellulitis (30.0\u00c2\u00a0%),<br \/>\n         and 3 were furuncles (10.0\u00c2\u00a0%), and the type of SSTI was undocumented in one case.<br \/>\n         13 of 30 (43.3\u00c2\u00a0%) recurrent infections met Centers for Disease Control and Prevention<br \/>\n         (CDC) criteria for a community-associated SSTI (CA-SSTI) 18]. The primary reason that an SSTI was not classified as a CA-SSTI was hospitalization<br \/>\n         within the prior year, which was the case in 12\/30 (40.0\u00c2\u00a0%) patients.\n      <\/p>\n<p>Culture data were only obtained for 8 of the recurrent SSTIs, and of those, 6 of the<br \/>\n         8 (75\u00c2\u00a0%) were confirmed <em>S. aureus<\/em> infections, with 4 of the 6 (67\u00c2\u00a0%) being MRSA. Of those 4 infections, 3 were clindamycin-susceptible<br \/>\n         MRSA, and all four were susceptible to trimethoprim-sulfamethoxazole. Of the 6 culture-proven<br \/><em>S. aureus<\/em> infections, only 1 MRSA SSTI met CDC criteria for being a CA-SSTI. The other two<br \/>\n         SSTIs were caused by Proteus and a coagulase negative staphylococcus species. Three<br \/>\n         of the six recurrent SSTIs caused by <em>S. aureus<\/em> were associated with culture data for the initial SSTI; all three initial SSTIs were<br \/>\n         caused by <em>S. aureus<\/em> as well. In two patients, both infections were causes by MRSA, and in one patient,<br \/>\n         both infections were causes by MSSA.\n      <\/p>\n<p>Therapy in cases of recurrent SSTI was with a beta-lactam in five cases (16.7\u00c2\u00a0%),<br \/>\n         combination therapy in seven cases (23.3\u00c2\u00a0%), clindamycin in four cases (13.3\u00c2\u00a0%), TMP-SMX<br \/>\n         in three cases (10\u00c2\u00a0%), levofloxacin in one case (3.3\u00c2\u00a0%), and vancomycin in one case<br \/>\n         (3.3\u00c2\u00a0%). Five patients (16.7\u00c2\u00a0%) received no systemic antibacterial therapy, and antibiotic<br \/>\n         therapy was not documented in four cases (13.3\u00c2\u00a0%).\n      <\/p>\n<h4>Predictors of Recurrent SSTI<\/h4>\n<p>The results of univariate Cox regression with possible predictors of SSTI are listed<br \/>\n         in Table\u00c2\u00a03. At any given time point, the presence of an intravascular catheter (HR 4.62; 95\u00c2\u00a0%<br \/>\n         confidence intervals [CI] 1.08-19.7; <em>p<\/em>?=?0.04), chronic liver disease (HR 2.89; 95\u00c2\u00a0% CI 1.00-8.35, <em>p<\/em>?=?0.05), and lymphedema (HR 4.12; 95\u00c2\u00a0% CI 1.24-14.1; <em>p<\/em>?=?0.02) were associated with an increased risk of recurrent SSTI, while African-American<br \/>\n         race was associated with decreased risk of recurrent SSTI (HR 0.34; 95\u00c2\u00a0% CI 0.11-1.00;<br \/><em>p<\/em>?=?0.05).<\/p>\n<p><strong>Table 3.<\/strong> Predictors of risk of recurrent SSTI in univariate and multivariate Cox regression<br \/>\n         models\n      <\/p>\n<p>Predictors with <em>p<\/em>??0.2 were candidates for the final multivariate Cox model, which was developed by<br \/>\n         a forward selection algorithm. Significant predictors as well as theoretical concerns<br \/>\n         led to the choice of our final model for multivariate regression. For example, we<br \/>\n         found a strong association between lymphedema and intravenous drug use (IVDU) in our<br \/>\n         cohort; we accordingly only included IVDU in the final model to avoid collinearity.<br \/>\n         Similarly, although gonorrhea was a strong statistical predictor of recurrent SSTI<br \/>\n         in several preliminary multivariate models, we found that models including gonorrhea<br \/>\n         were overly influenced by the single subject with a history of gonorrhea during follow<br \/>\n         up with recurrent SSTI (out of two subjects with a history of gonorrhea during follow<br \/>\n         up). Accordingly, gonorrhea was not included in the final model as it was felt that<br \/>\n         the data were inadequate to allow for a multivariable analysis including this predictor.<br \/>\n         Risk factors for recurrent SSTI in the final multivariable Cox regression model were<br \/>\n         non-hepatitis liver disease (HR 3.44; 95\u00c2\u00a0% CI 1.02-11.5; <em>p<\/em>?=?0.05), the presence of an intravenous catheter (HR 6.50; 95\u00c2\u00a0% CI 1.47-28.7; <em>p<\/em>?=?0.01), and a history of intravenous drug use (HR 2.80; 95\u00c2\u00a0% CI 1.02-7.65; <em>p<\/em>?=?0.05); African-American race remained associated with a decreased risk (HR 0.17;<br \/>\n         95\u00c2\u00a0% CI 0.05-0.54; <em>p<\/em>??0.01). A trend was present for HIV viral load ?1000 copies\/mL as an independent<br \/>\n         risk factor for recurrent SSTI (HR 2.21; 95\u00c2\u00a0% CI 0.99-4.94; <em>p<\/em>?=?0.05), which was nearly statistically significant. A Cox-Snell residual plot demonstrated<br \/>\n         that the model fit the data well (plot not shown).\n      <\/p>\n<p>As a sensitivity analysis, we repeated the above analyses but used 30-, 60-, 90- and<br \/>\n         365-day recent averages for a number of the above time-varying factors, without significant<br \/>\n         change in the results (data not shown). Similarly, we used linearly extrapolated CD4+<br \/>\n         counts and HIV VLs and found that point estimates did not change significantly. As<br \/>\n         a final sensitivity analysis, we used CD4+ count of 200 as an alternative cutoff,<br \/>\n         without significant change in the results.\n      <\/p>\n","protected":false},"excerpt":{"rendered":"<p>Population characteristics Of the 511 subjects in the initial cohort, 87 individuals (17.0\u00c2\u00a0%) experienced at least one SSTI, as described elsewhere 6]. Two subjects from the cohort had no follow-up time after the initial SSTI, so 85 subjects were included in the analysis reported in this study. The demographics of this cohort are shown in [&hellip;]<\/p>\n","protected":false},"author":1,"featured_media":0,"comment_status":"closed","ping_status":"closed","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[],"tags":[],"class_list":["post-26991","post","type-post","status-publish","format-standard","hentry"],"_links":{"self":[{"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/posts\/26991","targetHints":{"allow":["GET"]}}],"collection":[{"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/posts"}],"about":[{"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/types\/post"}],"author":[{"embeddable":true,"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/users\/1"}],"replies":[{"embeddable":true,"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/comments?post=26991"}],"version-history":[{"count":0,"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/posts\/26991\/revisions"}],"wp:attachment":[{"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/media?parent=26991"}],"wp:term":[{"taxonomy":"category","embeddable":true,"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/categories?post=26991"},{"taxonomy":"post_tag","embeddable":true,"href":"http:\/\/healthmedicinet.com\/news\/wp-json\/wp\/v2\/tags?post=26991"}],"curies":[{"name":"wp","href":"https:\/\/api.w.org\/{rel}","templated":true}]}}