Your search keyword '"Min B Thapa"' showing total 2 results

1. Safety and efficacy assessment of two new leprosy skin test antigens: randomized double blind clinical study

Author

Chaman Ranjit, Bishwa Raj Sapkota, Chhatra B. Kunwar, Patrick J. Brennan, Becky Rivoire, Eric Zhou, Robin Mason, Mark Wolff, Nathan A. Groathouse, RA Hawksworth, Christine Sizemore, Stephen TerLouw, Melinda Tibbals, Saraswoti Khadge, Mamodikoe Makhene, Min B Thapa, Dewei She, Murdo Macdonald, Tina Dube, Carol Smith, Kapil D. Neupane, and Deanna A. Hagge

Subjects

Male, Gastroenterology, law.invention, 0302 clinical medicine, Randomized controlled trial, law, Medicine and Health Sciences, 030212 general & internal medicine, Mycobacterium leprae, 0303 health sciences, biology, lcsh:Public aspects of medicine, Middle Aged, 3. Good health, Infectious Diseases, Research Design, Female, Leprosy, Research Article, Adult, medicine.medical_specialty, Tuberculosis, lcsh:Arctic medicine. Tropical medicine, Adolescent, Clinical Research Design, lcsh:RC955-962, Tuberculin, Research and Analysis Methods, Microbiology, Sensitivity and Specificity, Young Adult, 03 medical and health sciences, Double-Blind Method, Antigen, Internal medicine, medicine, Humans, Adverse effect, Skin Tests, 030304 developmental biology, Antigens, Bacterial, business.industry, Public Health, Environmental and Occupational Health, Biology and Life Sciences, lcsh:RA1-1270, medicine.disease, biology.organism_classification, Clinical trial, Immunology, business

Abstract

Background New tools are required for the diagnosis of pre-symptomatic leprosy towards further reduction of disease burden and its associated reactions. To address this need, two new skin test antigens were developed to assess safety and efficacy in human trials. Methods A Phase I safety trial was first conducted in a non-endemic region for leprosy (U.S.A.). Healthy non-exposed subjects (n = 10) received three titrated doses (2.5 µg, 1.0 µg and 0.1 µg) of MLSA-LAM (n = 5) or MLCwA (n = 5) and control antigens [Rees MLSA (1.0 µg) and saline]. A randomized double blind Phase II safety and efficacy trial followed in an endemic region for leprosy (Nepal), but involved only the 1.0 µg (high dose) and 0.1 µg (low dose) of each antigen; Tuberculin PPD served as a control antigen. This Phase II safety and efficacy trial consisted of three Stages: Stage A and B studies were an expansion of Phase I involving 10 and 90 subjects respectively, and Stage C was then conducted in two parts (high dose and low dose), each enrolling 80 participants: 20 borderline lepromatous/lepromatous (BL/LL) leprosy patients, 20 borderline tuberculoid/tuberculoid (BT/TT) leprosy patients, 20 household contacts of leprosy patients (HC), and 20 tuberculosis (TB) patients. The primary outcome measure for the skin test was delayed type hypersensitivity induration. Findings In the small Phase I safety trial, reactions were primarily against the 2.5 µg dose of both antigens and Rees control antigen, which were then excluded from subsequent studies. In the Phase II, Stage A/B ramped-up safety study, 26% of subjects (13 of 50) showed induration against the high dose of each antigen, and 4% (2 of 50) reacted to the low dose of MLSA-LAM. Phase II, Stage C safety and initial efficacy trial showed that both antigens at the low dose exhibited low sensitivity at 20% and 25% in BT/TT leprosy patients, but high specificity at 100% and 95% compared to TB patients. The high dose of both antigens showed lower specificity (70% and 60%) and sensitivity (10% and 15%). BL/LL leprosy patients were anergic to the leprosy antigens. Interpretation MLSA-LAM and MLCwA at both high (1.0 µg) and low (0.1 µg) doses were found to be safe for use in humans without known exposure to leprosy and in target populations. At a sensitivity rate of 20–25% these antigens are not suitable as a skin test for the detection of the early stages of leprosy infection; however, the degree of specificity is impressive given the presence of cross-reactive antigens in these complex native M. leprae preparations. Trial Registration ClinicalTrails.gov NCT01920750 (Phase I), NCT00128193 (Phase II), Author Summary Clinically useful skin test reagents should be safe and sufficiently sensitive to detect infection prior to physical manifestations of leprosy disease. While in these small scale human studies, leprosy reagents were safe for use in humans, they failed in respect of sensitivity at a rate of 20–25% in the key indicator group, BT/TT leprosy patients. Specificity in terms of leprosy vs. tuberculosis at a rate of 95–100% was surprisingly high in light of the extensive presence of cross-reactive antigens in the complex native M. leprae preparations. These results could justify a further trial at lower dosages.

Published

2014

2. Diagnosis and treatment of leprosy reactions in integrated services--the patients' perspective in Nepal

Author

Diana N. J. Lockwood, Saraswoti Khadge, Min B Thapa, Krishna Bahadur Tamang, Sonia F. Raffe, and Deanna A. Hagge

Subjects

myalgia, Adult, Male, medicine.medical_specialty, lcsh:Arctic medicine. Tropical medicine, Referral, Adolescent, Service delivery framework, lcsh:RC955-962, MEDLINE, Physical examination, Interviews as Topic, Young Adult, Nepal, Leprosy, medicine, Humans, Young adult, Aged, medicine.diagnostic_test, business.industry, lcsh:Public aspects of medicine, Public Health, Environmental and Occupational Health, Health services research, lcsh:RA1-1270, Middle Aged, medicine.disease, Hospitals, Infectious Diseases, Family medicine, Physical therapy, Medicine, Female, Health Services Research, medicine.symptom, business, Delivery of Health Care, Research Article, Neglected Tropical Diseases

Abstract

Leprosy care has been integrated with peripheral health services, away from vertical programmes. This includes the diagnosis and management of leprosy reactions, which cause significant morbidity. We surveyed patients with leprosy reactions at two leprosy hospitals in Nepal to assess their experience of leprosy reaction management following integration to identify any gaps in service delivery. Methods Direct and referral patients with leprosy reactions were interviewed in two of Nepal's leprosy hospitals. We also collected quantitative and qualitative data from clinical examination and case-note review to document the patient pathway. Results Seventy-five patients were interviewed. On development of reaction symptoms 39% presented directly to specialist services, 23% to a private doctor, 17% to a district hospital, 10% to a traditional healer, 7% to a health post and 4% elsewhere. Those who presented directly to specialist services were 6.6 times more likely to start appropriate treatment than those presenting elsewhere (95% CI: 3.01 to 14.45). The average delay between symptom onset to commencing corticosteroids was 2.9 months (range 0–24 months). Obstacles to early presentation and treatment included diagnostic challenge, patients' lack of knowledge and the patients' view of health as a low priority. 40% received corticosteroids for longer than 12 weeks and 72% required an inpatient stay. Treatment follow-up was conducted at locations ranging from health posts to specialist hospitals. Inconsistency in the availability of corticosteroids peripherally was identified and 41% of patients treated for leprosy and a reaction on an outpatient basis attended multiple sites for follow-up treatment. Conclusion This study demonstrates that specialist services are necessary and continue to provide significant critical support within an integrated health system approach towards the diagnosis and management of leprosy reactions., Author Summary The global strategy for leprosy has moved patient care to general health services with the aim of improving access to treatment. We suspected that leprosy patients with a common complication, leprosy reactions, are not being diagnosed and treated promptly in integrated services. Leprosy reactions cause nerve damage and, if not treated early, can cause significant disability. We interviewed 75 patients with a leprosy reaction in Nepal, a country with a fully-integrated leprosy service. Patients were experiencing average delays of 2.9 months between developing leprosy reactions and starting treatment. Many required extended courses of treatment, an inpatient stay or experienced a recurrence of their reaction. Patients also continue to attend specialist services for both diagnosis and follow-up. Patient care could be improved by utilising specialist knowledge for training and the management of complex cases. Health care workers and patients need to be educated about leprosy reactions. A wider implication of the study is that health policy-makers need to be cautious not to over-simplify medical conditions when restructuring services.

Published

2013