Good estimates for the number of coinfected persons actually accessing care are not available. The only available data relate to the Province of Ontario, where approximately 65% of persons diagnosed with HIV have accessed care at least once (defined as having at least one HIV viral load measurement after diagnosis), whereas only 51% can be said to be in regular medical follow-up [17]. Thus, the 955 cohort participants probably represent close to 20% of all coinfected patients receiving

treatment in Canada. We have provided a comprehensive picture of the extent of vulnerabilities that present challenges to effective care and prevention of serious morbidity and mortality in this population. There are extremely high rates of social

instability, poverty, mental illness and alcohol and drug use. www.selleckchem.com/products/torin-1.html Aboriginals are disproportionately represented in our cohort. Whereas they comprised 3.8% of the Canadian population in 2006 and 8% of prevalent HIV infections [18], 15% of our cohort overall and 33% in British Columbia self-identified as aboriginal and a very high proportion of these were women (62%). The impact of these combined vulnerabilities on the health of the coinfected population appears Aurora Kinase inhibitor to be appreciable. Despite 82% of participants in the cohort receiving ART, only 71% were virologically suppressed. Another 6% had interrupted treatment at baseline. While these results are not dissimilar from those of other studies in IDU populations, these viral suppression rates are lower than those reported generally in HIV-infected persons [19-21]. Together, our results highlight that a significant proportion of participants Adenosine triphosphate have difficulty with treatment adherence and consequently are at risk for developing viral resistance and experiencing HIV-related disease progression. Indeed, the rate of AIDS was very high, at twice the reported

rate in a US HIV-infected population for the period 2003–2007 [22]. Incomplete HIV suppression may also have implications for HIV transmission, especially given the high percentage of participants that report sharing injection equipment and risky sexual behaviours. Finally, treatment interruptions have also been associated with increased risk for non-AIDS-related adverse outcomes, including liver disease progression and death, particularly among coinfected persons [23, 24]. HCV infection is a chronic infection which if left untreated follows a slow clinical course progressing to ESLD and hepatocellular carcinoma [25]. HIV increases chronicity and accelerates the natural history of HCV [7, 26]. This impact is mirrored in our cohort: the median age of the population and time since HCV infection suggest that we are poised for a peak of chronic liver disease and its consequences. Indeed, at baseline many participants already had significant fibrosis and ESLD.