Colin Terry
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Medicine | 2018
Joseph Wheat; Thein Myint; Ying Guo; Phebe Kemmer; Chadi A. Hage; Colin Terry; Marwan M. Azar; James Riddell; Peter T. Ender; S. Chen; Kareem W. Shehab; Kerry O. Cleveland; Eden Esguerra; James G. Johnson; Patty Wright; Vanja C. Douglas; Pascalis Vergidis; Winnie W. Ooi; John W. Baddley; David M. Bamberger; Raed N Khairy; Holenarasipur R. Vikram; Elizabeth R. Jenny-Avital; Geetha Sivasubramanian; Karen L. Bowlware; Barbara Pahud; Juan C. Sarria; Townson Tsai; Maha Assi; Satish Mocherla
Abstract Central nervous system (CNS) involvement occurs in 5 to 10% of individuals with disseminated histoplasmosis. Most experience has been derived from small single center case series, or case report literature reviews. Therefore, a larger study of central nervous system (CNS) histoplasmosis is needed in order to guide the approach to diagnosis, and treatment. A convenience sample of 77 patients with histoplasmosis infection of the CNS was evaluated. Data was collected that focused on recognition of infection, diagnostic techniques, and outcomes of treatment. Twenty nine percent of patients were not immunosuppressed. Histoplasma antigen, or anti-Histoplasma antibodies were detected in the cerebrospinal fluid (CSF) in 75% of patients. One year survival was 75% among patients treated initially with amphotericin B, and was highest with liposomal, or deoxycholate formulations. Mortality was higher in immunocompromised patients, and patients 54 years of age, or older. Six percent of patients relapsed, all of whom had the acquired immunodeficiency syndrome (AIDS), and were poorly adherent with treatment. While CNS histoplasmosis occurred most often in immunocompromised individuals, a significant proportion of patients were previously, healthy. The diagnosis can be established by antigen, and antibody testing of the CSF, and serum, and antigen testing of the urine in most patients. Treatment with liposomal amphotericin B (AMB-L) for at least 1 month; followed by itraconazole for at least 1 year, results in survival among the majority of individuals. Patients should be followed for relapse for at least 1 year, after stopping therapy.
Journal of Religion & Health | 2008
Paul S. Bay; Daniel Beckman; James Trippi; Richard B. Gunderman; Colin Terry
American Journal of Obstetrics and Gynecology | 2005
Carlos A Labarrere; M.A. Ortiz; Marcelo J. Sosa; G.L. Campana; Mario Wernicke; Lee Ann Baldridge; Colin Terry; Hector L. DiCarlo
Holistic Nursing Practice | 2010
Paul S. Bay; Steven S. Ivy; Colin Terry
Journal of Heart and Lung Transplantation | 2006
C.A. Labarrere; M.A. Ortiz; Nargiz Ruzmetov; Marcelo J. Sosa; G.L. Campana; Colin Terry; Lee Ann Baldridge; Roula Antonopoulos; Hector L. DiCarlo
Journal of Heart and Lung Transplantation | 2007
C.A. Labarrere; G.L. Campana; George Boguslawski; M.A. Ortiz; Marcelo J. Sosa; Colin Terry; D.E. Pitts; J.A. O’Donnell; D.A. Hormuth
Journal of Heart and Lung Transplantation | 2006
C.A. Labarrere; M.A. Ortiz; Nargiz Ruzmetov; Marcelo J. Sosa; G.L. Campana; Colin Terry; Lee Ann Baldridge; Roula Antonopoulos; Hector L. DiCarlo
Journal of Heart and Lung Transplantation | 2006
C.A. Labarrere; M.A. Ortiz; G.L. Campana; Marcelo J. Sosa; Colin Terry; D.E. Pitts; D.A. Hormuth; Mario C. Deng
Journal of Heart and Lung Transplantation | 2005
C.A. Labarrere; M.A. Ortiz; Hector L. DiCarlo; G.L. Campana; Marcelo J. Sosa; Colin Terry; D.E. Pitts; D.A. Hormuth; Mario C. Deng
Journal of Heart and Lung Transplantation | 2004
C.A. Labarrere; Hector L. DiCarlo; M.A. Ortiz; Colin Terry; D.E. Pitts; D.A. Hormuth