The records at our stem-cell transplantation centre were reviewed to identify the patients who underwent autologous HSCT between April 2009 and December 2010. Patients
were classified as having proven invasive aspergillosis (IA), probable IA, or possible IA on the basis of the criteria established by the European Organization for Research and Treatment of Cancer and Mycoses Study Group (independent of the BDG results). During the study period, the patients were screened for BDG twice a week from transplant (day 0) until engraftment. Three patients were diagnosed with probable IA and five were diagnosed with possible IA. A total of 354 serum Selleckchem NVP-AUY922 samples from79 patients who met the study inclusion criteria were used for statistical analysis. At the cut-off value of 80 pg ml−1, the sensitivity was 27.2% [95% confidence interval (CI); 7.3–60.6]; specificity, 94.4% (95% CI; 91.3–96.5); positive predictive value, 6.2%; and negative predictive, 93.7%. The clinical contribution find more of the BDG assay as a screening test was relatively limited in this cohort of patients undergoing autologous HSCT. “
“Centre for Microbial Biotechnology,
Panjab University, Chandigarh, India Mucormycosis remains a devastating invasive fungal infection, with high mortality rates even after Oxymatrine active management. The disease is being reported at an alarming frequency over the past decades from India. Indian mucormycosis has certain unique features. Rhino-orbito-cerebral presentation associated with uncontrolled diabetes is the predominant characteristic. Isolated renal mucormycosis has emerged as a new clinical entity. Apophysomyces elegans and Rhizopus
homothallicus are emerging species in this region and uncommon agents such as Mucor irregularis and Thamnostylum lucknowense are also being reported. This review focuses on these distinct features of mucormycosis observed in India. Fungi belonging to the class Zygomycetes and order Mucorales often cause devastating angioinvasive fungal infections, primarily in patients with underlying risk factors.[1] These moulds gain entry into the human body via respiratory tract or skin, and less commonly through the gastrointestinal tract, eliciting an acute inflammatory response.[2] Under favourable conditions such as those in immunocompromised hosts, they invade the blood vessels, causing extensive vessel thrombosis and ischaemic tissue necrosis.[2, 3] Most of these infections are rapidly progressive and exhibit high mortality (~50%) even after active management; the mortality rates approach nearly 100% among patients with disseminated disease.