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1. OVERDOSE MEDICAMENTOSA POR PARACETAMOL E OPIÓIDES: REPERCUSSÕES E TRATAMENTOS

Author

SANTOS, VITÓRIA HAGGE DA SILVA, primary, FRANÇA, BRENO PAIVA LEMOS GALVÃO DE, additional, and ANDRÉ, MARIA LUIZA PINTO, additional

Published

2022

2. Saúde da Mulher - volume 1

Author

Fonseca, Cyro Vilela da, primary, Cavalheiro, Beatriz Pyrich, additional, Romanini, Aline Puzzi, additional, Silva, Mariana Xavier e, additional, Nieto, Gislayne Castro e Souza, additional, Brito, Patrícia Leite, additional, INNOCENTE, MARIA LAURA BRUNELLI, additional, MORAES, BRUNA DE MOURA, additional, Gama, Maria Gracimar Fecury da, additional, Teixeira, Matheus Diniz, additional, Silva, Larissa de Andrade, additional, Nunes, Suzana Carvalho, additional, Goulart, Jéssica, additional, Gelatti, Gabriela Tassotti, additional, Felippin, Tamiris, additional, Mayer, Mariana Spanamberg, additional, Tissiani, Ana Caroline, additional, Heringer, Tiago Antonio, additional, Thums, Isis Amaral, additional, Calçada, João Pedro Cunha, additional, Alegransi, Caroline, additional, Bonfanti, Gabriela, additional, Golle, Diego Pascoal, additional, Cattaneo, Roberta, additional, Barbosa, Alicy Verônica Alves, additional, Talim, Amanda Torres, additional, Braga, Henrique Drumond, additional, Gatti, Júlia Domingues, additional, Avelar, Luiza Magalhães, additional, Azevedo, Mariana de Oliveira, additional, Pinto, Matheus Pires, additional, Castro, Patrícia Maria Carneiro de, additional, Nunes, Paula Braga, additional, Gatti, Paula Domingues, additional, Silva, Raphaela Ilmara Campos Duque da, additional, Ferreira, Sibelly Vaz de Mello Loureiro, additional, Alves, Débora Pimenta, additional, Annuzzo, Miguel de Sousa e, additional, Camargo, Juliana Bretas, additional, Sa, Marcio Erlei Vieira de, additional, Lima, Rafael Lauro Silva, additional, Moreira, Fernanda Assis Vieira, additional, Freitas, Adriana Ruphael de, additional, Canuto, Amanda Beatriz Oliveira, additional, Santos, Amanda de Oliveira, additional, Reis, Amanda Lílici Valle, additional, Matos, Amanda Soares, additional, Viana, Ana Beatriz Almeida, additional, Botelho, Ana Beatriz Nogueira, additional, Ferreira, Ana Elisa de Castro, additional, Coelho, Ana Luísa Loschi, additional, Carvalho, Bianca Silva de, additional, Oliveira, Dulcilene Mayrink de, additional, Canuto, André Luis, additional, Costa, José Orleans da, additional, Trigueiro, Gustavo Machado, additional, Carvalho, Ana Júlia, additional, Moreira, Geovanna Karolliny Marques, additional, Silva, Nardel Luiz Ribeiro da, additional, Nascimento, Natália Leite, additional, Peres, Paula Moreira, additional, Costa, Carla Danielle Dias, additional, Innocente, Maria Laura Brunelli, additional, Moraes, Bruna de Moura, additional, Acioli, Rebeca Vital Matias, additional, Formiga, Aline Cristina Abrantes, additional, Queiroz, Carolina Travassos de, additional, França, Iannah Mendonça Freire de, additional, Maior, Luísa Vieira Souto, additional, Souza, Monise Santos, additional, Campos, Cássia Roberta Silva, additional, Mecenas, Jeanne Martins, additional, Lima, Patrícia Lopes de, additional, Nascimento, Synnara Mohana Alves do, additional, Mendes, Aumeires de Jesus Abreu, additional, Sousa, Fernanda Italiano Alves Benício, additional, Fontenele, Rafael Mondego, additional, Boechat, Esther Pifano, additional, Freitas, Caroline Martins de, additional, Ribeiro, Kalíli Danieli Barra, additional, Santos, Larissa Emy, additional, Ferreira, Wellington de Jesus, additional, Baêta, Gabriela Picchioni, additional, Bárbara, Mariana Azevedo Santa, additional, Souza, Dirceu Sander Correa de, additional, Porto, Daniella Patrícia de Oliveira, additional, Sâmia, Ana Eliza Ribeiro, additional, Oliveira, Nathan Shuenck Silva de, additional, Horta, Samuel Oliveira Dumont, additional, Teixeira, Micaella Ramos, additional, Horta, Sara Oliveira Dumont, additional, CORREIA, ELISA DE CASTRO, additional, CASTRO, ANA BEATRIZ SAMPAIO PINTO DE, additional, LIMA, TATIANA MONTANDON LASSI LOPES, additional, SILVA, HELLEN CAROLINA BRANDÃO, additional, BICALHO, GABRIELA BOLLER, additional, BERNIS, EDUARDA HERINGER, additional, BARBOSA, JOÃO ARTHUR RODRIGUES, additional, AZEVEDO, INGRIDY MARIA DINIZ MELO, additional, BICHARA, MATHEUS MIRANDA, additional, OLIVEIRA, RAYANA VIEGAS, additional, Gomes, Pedro Vinícius Teles, additional, Moreira, Anna Luiza Gonçalves, additional, Abreu, Gabriel Sousa de Freitas, additional, Gonçalves, Amanda Carolina de Melo, additional, Silva, Bárbara Leite da, additional, Dias, Karolinne Dorneles, additional, Costa, Anna Laura Caetano, additional, Puglia, Ana C, additional, Carvalho, Lanna C, additional, Batista, Matheus Neres, additional, Veloso, Eliana A N, additional, S, Joel A, additional, Monteiro, Dafny Rocha, additional, Nagahama, Camilla de Souza, additional, Nogueira, Giovana Pazotti, additional, Mendonça, Isabella Davo de, additional, Monteiro, Felipe Rocha, additional, Coutinho, Raphel Cândido Sepúlveda, additional, Monteiro, José Maury do Carmo, additional, Monteiro, Rosângela Lucinda Rocha, additional, Nora, Ana Paula de Oliveira, additional, Campos, Kamila Prado, additional, Bonfim, Bruna Rezende, additional, Kamel, Milena Freire Abu, additional, Silva, Rayanne Christina, additional, Machado, Laura Castanheira, additional, Teixeira, Ana Laura Mesquita, additional, Debossan, Lívia Costa, additional, Reche, Giovana Bellettato, additional, Assis, Izabelle Rezende de, additional, Morais, Bárbara Catão Ferreira de, additional, Castanheira, Eliana Motta, additional, Antonio, Sabrina de Carvalho, additional, ALMEIDA, JULIANA VIEIRA QUEIROZ, additional, Amorim, Arthur Donato, additional, Pimenta, Camila de Melo, additional, Monteiro, Yolanda Talissa, additional, Pereira, Maria Clara Leal, additional, Silva, Felipe André Sousa, additional, Nunes, Bruna Lorena Meneses, additional, Lobo, Luis Henrique Dias, additional, Moura, Sâmia Gonçalves de, additional, Silva, Pedro Henrique Freitas, additional, Leal, Antonia Lucimary de Sousa, additional, Leal, Victor César Gonçalves Barros, additional, Leal, Lucas Luan Gonçalves Barros, additional, Monteiro, André Felipe Cardoso, additional, Lemos, Thaís da Silva Alves de, additional, Silva, Maria Arniele Pereira, additional, Silva, Lissa Lavínia de Oliveira, additional, Cavalcanti, Rayane Chagas, additional, silva, Franciare vieira, additional, Silva, Lísia Marília Tenório da, additional, Macêdo, Luanna Calado de, additional, Lima, Mayra Bianca Lopes, additional, Salviano, Iara Fernanda as Silva, additional, Rocha, Ana Claúdia Gomes da Hora, additional, santos, Marcela Farias dos, additional, Silva, Rayane Soares da, additional, Metz, Soraya Katine Garcia, additional, Pensin, Taiana Grespan, additional, Bortolini, Michele Fernanda, additional, Takase, Marisiane Alves Carneiro, additional, Hartmann, Adriana, additional, Santos, Edilson Lima dos, additional, Silvestri, Aline Paula Spibida, additional, Belini, Gabriela Fagan, additional, Pellizzaro, André Olivo, additional, Moura, Tamíres da Silva, additional, Gonçalves, Suelen, additional, Silva, Carlos Roberto Gomes da, additional, Cavalcanti, Bianca Brunet, additional, Jatobá, Rafaela Souto Maior, additional, Lombardi, Maria Eduarda Medeiros, additional, Lima, Rodrigo Lourenço Bulhões, additional, Damasceno, André Barreto, additional, Brito, Isadora Pereira, additional, Rocha, Maria Fernanda Stuart Holmes, additional, Carvalho, Lucas Fernandes de Queiroz, additional, Queiroz, João Vicente Jales de, additional, Moscardini, Maria Cecília de Paula, additional, Candido, Milenny Fernanda Vasconcelos, additional, Sousa, Ana Carolina Soares, additional, Rios, Marcella Maciel, additional, SPÓSITO, LAVÍNIA ARRUDA, additional, Carvalho, Lanna do Carmo, additional, Araújo, Vitória Gabriele Barros de, additional, SANTOS, JEHOVAHNNA ANTTONIONI, additional, Pinheiro, Elisama Pereira, additional, Carlos, Igor Henrique Silva, additional, Vieira, Ana Júlia, additional, Sousa, Joel Alves de, additional, Silva, Angellita de Kássya Ferreira da, additional, Sousa, Thaysia Moura dos Santos, additional, Mendes, Polyana Norberta, additional, Araújo, Lavínia B, additional, Mata, Alicce Abreu da, additional, Dias, Isabela Karina Silva, additional, Almeida, Isadora Velloso de, additional, Pizzamiglio, Julia Cardozo, additional, Silva, Lucas Gláucio da, additional, Franqueira, Nayara Coli de Paiva, additional, Vicente, Patrícia Tambasco Freire, additional, Motta, Paula Delgado Machado Henriques, additional, Santos, Vitória Hagge da Silva, additional, Figueiredo, Ana Cláudia Dias Sousa, additional, Holanda, Sarah Maria Monteiro Soares Costa de, additional, Almeida, Adisânia Araújo de, additional, Gramosa, Ana Flávia Policarpo, additional, Policarpo, Elayne Ester Nogueira Santos, additional, Sousa, Evanayza Vieira de, additional, Rêgor, Gustavo Zannata Cronemberger de Ferraz, additional, Ungarelli, Isabella Mota, additional, Mourthé, Victoria Cristina Guimarães Pedras, additional, Oliveira, Isabela Ferreira Estevam de, additional, Alves, Camila Sousa Bragunce, additional, Tuyama, Marina Gontijo, additional, Carvalho, Gabriela Dantas, additional, Silva, Marcélia Gomes, additional, Sobrinho, Bianca Gisele Lira Gonzaga, additional, Silva, Eulália Luana Rodrigues da, additional, Castro, Juçara Gonçalves de, additional, Barroso, Guilherme, additional, Brito, Sara Ferreira Lobato de, additional, Rocha, Valéria Alves da, additional, Pereira, Edla Sindy Alves Ferreira, additional, Brito, Patricia Leite, additional, Barcellos, Lavinia, additional, Fonseca, Cyro Vilela da, additional, Salviano, Iara Fernanda da Silva, additional, Oliveira, Edilson Josué de, additional, and Neves, Silvana Maria Véras, additional

Published

2021

3. OVERDOSE MEDICAMENTOSA POR PARACETAMOL E OPIÓIDES: REPERCUSSÕES E TRATAMENTOS

Author

VITÓRIA HAGGE DA SILVA SANTOS, BRENO PAIVA LEMOS GALVÃO DE FRANÇA, and MARIA LUIZA PINTO ANDRÉ

Published

2022

4. Saúde da Mulher - volume 1

Author

Cyro Vilela da Fonseca, Beatriz Pyrich Cavalheiro, Aline Puzzi Romanini, Mariana Xavier e Silva, Gislayne Castro e Souza Nieto, Patrícia Leite Brito, MARIA LAURA BRUNELLI INNOCENTE, BRUNA DE MOURA MORAES, Maria Gracimar Fecury da Gama, Matheus Diniz Teixeira, Larissa de Andrade Silva, Suzana Carvalho Nunes, Jéssica Goulart, Gabriela Tassotti Gelatti, Tamiris Felippin, Mariana Spanamberg Mayer, Ana Caroline Tissiani, Tiago Antonio Heringer, Isis Amaral Thums, João Pedro Cunha Calçada, Caroline Alegransi, Gabriela Bonfanti, Diego Pascoal Golle, Roberta Cattaneo, Alicy Verônica Alves Barbosa, Amanda Torres Talim, Henrique Drumond Braga, Júlia Domingues Gatti, Luiza Magalhães Avelar, Mariana de Oliveira Azevedo, Matheus Pires Pinto, Patrícia Maria Carneiro de Castro, Paula Braga Nunes, Paula Domingues Gatti, Raphaela Ilmara Campos Duque da Silva, Sibelly Vaz de Mello Loureiro Ferreira, Débora Pimenta Alves, Miguel de Sousa e Annuzzo, Juliana Bretas Camargo, Marcio Erlei Vieira de Sa, Rafael Lauro Silva Lima, Fernanda Assis Vieira Moreira, Adriana Ruphael de Freitas, Amanda Beatriz Oliveira Canuto, Amanda de Oliveira Santos, Amanda Lílici Valle Reis, Amanda Soares Matos, Ana Beatriz Almeida Viana, Ana Beatriz Nogueira Botelho, Ana Elisa de Castro Ferreira, Ana Luísa Loschi Coelho, Bianca Silva de Carvalho, Dulcilene Mayrink de Oliveira, André Luis Canuto, José Orleans da Costa, Gustavo Machado Trigueiro, Ana Júlia Carvalho, Geovanna Karolliny Marques Moreira, Nardel Luiz Ribeiro da Silva, Natália Leite Nascimento, Paula Moreira Peres, Carla Danielle Dias Costa, Maria Laura Brunelli Innocente, Bruna de Moura Moraes, Rebeca Vital Matias Acioli, Aline Cristina Abrantes Formiga, Carolina Travassos de Queiroz, Iannah Mendonça Freire de França, Luísa Vieira Souto Maior, Monise Santos Souza, Cássia Roberta Silva Campos, Jeanne Martins Mecenas, Patrícia Lopes de Lima, Synnara Mohana Alves do Nascimento, Aumeires de Jesus Abreu Mendes, Fernanda Italiano Alves Benício Sousa, Rafael Mondego Fontenele, Esther Pifano Boechat, Caroline Martins de Freitas, Kalíli Danieli Barra Ribeiro, Larissa Emy Santos, Wellington de Jesus Ferreira, Gabriela Picchioni Baêta, Mariana Azevedo Santa Bárbara, Dirceu Sander Correa de Souza, Daniella Patrícia de Oliveira Porto, Ana Eliza Ribeiro Sâmia, Nathan Shuenck Silva de Oliveira, Samuel Oliveira Dumont Horta, Micaella Ramos Teixeira, Sara Oliveira Dumont Horta, ELISA DE CASTRO CORREIA, ANA BEATRIZ SAMPAIO PINTO DE CASTRO, TATIANA MONTANDON LASSI LOPES LIMA, HELLEN CAROLINA BRANDÃO SILVA, GABRIELA BOLLER BICALHO, EDUARDA HERINGER BERNIS, JOÃO ARTHUR RODRIGUES BARBOSA, INGRIDY MARIA DINIZ MELO AZEVEDO, MATHEUS MIRANDA BICHARA, RAYANA VIEGAS OLIVEIRA, Pedro Vinícius Teles Gomes, Anna Luiza Gonçalves Moreira, Gabriel Sousa de Freitas Abreu, Amanda Carolina de Melo Gonçalves, Bárbara Leite da Silva, Karolinne Dorneles Dias, Anna Laura Caetano Costa, Ana C Puglia, Lanna C Carvalho, Matheus Neres Batista, Eliana A N Veloso, Joel A S, Dafny Rocha Monteiro, Camilla de Souza Nagahama, Giovana Pazotti Nogueira, Isabella Davo de Mendonça, Felipe Rocha Monteiro, Raphel Cândido Sepúlveda Coutinho, José Maury do Carmo Monteiro, Rosângela Lucinda Rocha Monteiro, Ana Paula de Oliveira Nora, Kamila Prado Campos, Bruna Rezende Bonfim, Milena Freire Abu Kamel, Rayanne Christina Silva, Laura Castanheira Machado, Ana Laura Mesquita Teixeira, Lívia Costa Debossan, Giovana Bellettato Reche, Izabelle Rezende de Assis, Bárbara Catão Ferreira de Morais, Eliana Motta Castanheira, Sabrina de Carvalho Antonio, JULIANA VIEIRA QUEIROZ ALMEIDA, Arthur Donato Amorim, Camila de Melo Pimenta, Yolanda Talissa Monteiro, Maria Clara Leal Pereira, Felipe André Sousa Silva, Bruna Lorena Meneses Nunes, Luis Henrique Dias Lobo, Sâmia Gonçalves de Moura, Pedro Henrique Freitas Silva, Antonia Lucimary de Sousa Leal, Victor César Gonçalves Barros Leal, Lucas Luan Gonçalves Barros Leal, André Felipe Cardoso Monteiro, Thaís da Silva Alves de Lemos, Maria Arniele Pereira Silva, Lissa Lavínia de Oliveira Silva, Rayane Chagas Cavalcanti, Franciare vieira silva, Lísia Marília Tenório da Silva, Luanna Calado de Macêdo, Mayra Bianca Lopes Lima, Iara Fernanda as Silva Salviano, Ana Claúdia Gomes da Hora Rocha, Marcela Farias dos santos, Rayane Soares da Silva, Soraya Katine Garcia Metz, Taiana Grespan Pensin, Michele Fernanda Bortolini, Marisiane Alves Carneiro Takase, Adriana Hartmann, Edilson Lima dos Santos, Aline Paula Spibida Silvestri, Gabriela Fagan Belini, André Olivo Pellizzaro, Tamíres da Silva Moura, Suelen Gonçalves, Carlos Roberto Gomes da Silva, Bianca Brunet Cavalcanti, Rafaela Souto Maior Jatobá, Maria Eduarda Medeiros Lombardi, Rodrigo Lourenço Bulhões Lima, André Barreto Damasceno, Isadora Pereira Brito, Maria Fernanda Stuart Holmes Rocha, Lucas Fernandes de Queiroz Carvalho, João Vicente Jales de Queiroz, Maria Cecília de Paula Moscardini, Milenny Fernanda Vasconcelos Candido, Ana Carolina Soares Sousa, Marcella Maciel Rios, LAVÍNIA ARRUDA SPÓSITO, Lanna do Carmo Carvalho, Vitória Gabriele Barros de Araújo, JEHOVAHNNA ANTTONIONI SANTOS, Elisama Pereira Pinheiro, Igor Henrique Silva Carlos, Ana Júlia Vieira, Joel Alves de Sousa, Angellita de Kássya Ferreira da Silva, Thaysia Moura dos Santos Sousa, Polyana Norberta Mendes, Lavínia B Araújo, Alicce Abreu da Mata, Isabela Karina Silva Dias, Isadora Velloso de Almeida, Julia Cardozo Pizzamiglio, Lucas Gláucio da Silva, Nayara Coli de Paiva Franqueira, Patrícia Tambasco Freire Vicente, Paula Delgado Machado Henriques Motta, Vitória Hagge da Silva Santos, Ana Cláudia Dias Sousa Figueiredo, Sarah Maria Monteiro Soares Costa de Holanda, Adisânia Araújo de Almeida, Ana Flávia Policarpo Gramosa, Elayne Ester Nogueira Santos Policarpo, Evanayza Vieira de Sousa, Gustavo Zannata Cronemberger de Ferraz Rêgor, Isabella Mota Ungarelli, Victoria Cristina Guimarães Pedras Mourthé, Isabela Ferreira Estevam de Oliveira, Camila Sousa Bragunce Alves, Marina Gontijo Tuyama, Gabriela Dantas Carvalho, Marcélia Gomes Silva, Bianca Gisele Lira Gonzaga Sobrinho, Eulália Luana Rodrigues da Silva, Juçara Gonçalves de Castro, Guilherme Barroso, Sara Ferreira Lobato de Brito, Valéria Alves da Rocha, Edla Sindy Alves Ferreira Pereira, Patricia Leite Brito, Lavinia Barcellos, Iara Fernanda da Silva Salviano, Edilson Josué de Oliveira, and Silvana Maria Véras Neves

Published

2021

5. Terapia hormonal no climatério como fator de risco para o desenvolvimento de câncer de mama e seus impactos na qualidade de vida

Author

Dias, Pedro Antonio Rodrigues, primary, Bussarello, Caroline, additional, Costa, Gabriela Cordeiro, additional, Vilela, Gabriella Rocha, additional, Roehrig, Júlia Bortolini, additional, Nasser, Luana Veiga da Silva, additional, Leandro, Mayara dos Santos, additional, Rahin, Samya Mohamed Abdul, additional, Santos, Vitória Hagge da Silva, additional, and Guimarães, Raquel Meirelles Gaspar Coelho, additional

Published

2021

6. Terapia hormonal no climatério como fator de risco para o desenvolvimento de câncer de mama e seus impactos na qualidade de vida

Author

Pedro Antonio Rodrigues Dias, Caroline Bussarello, Gabriela Cordeiro Costa, Gabriella Rocha Vilela, Júlia Bortolini Roehrig, Luana Veiga da Silva Nasser, Mayara dos Santos Leandro, Samya Mohamed Abdul Rahin, Vitória Hagge da Silva Santos, and Raquel Meirelles Gaspar Coelho Guimarães

Subjects

General Medicine

Abstract

Objetivo: Analisar, por meio de uma revisão narrativa, o impacto do uso da Terapia hormonal (TH) na qualidade de vida de mulheres no climatério e como fator de risco para o desenvolvimento do câncer de mama, bem como discutir as opções terapêuticas existentes, levando em consideração a melhoria na qualidade de vida das pacientes. Revisão Bibliográfica: A menopausa caracteriza o fim do período reprodutivo da mulher, com diminuição da atividade folicular ovariana. Esse período é marcado por instabilidades hormonais e sintomatologia marcante que faz com que muitas mulheres procurem a TH como forma de tratamento. Entretanto, a TH pode acometer o tecido mamário e resultar em uma neoplasia, a depender da formulação e do tempo de uso, além de possíveis fatores de risco para câncer de mama. Considerações finais: Conclui-se que a terapia hormonal está associada ao aumento do risco de desenvolvimento do câncer de mama, sendo esse risco atribuído, principalmente, aos progestagênios medroxiprogesterona, noretisterona e levonorgestrel. A descontinuação do uso destes tende a diminuir os riscos e, de uma forma geral, a sua administração não é recomendada por período superior a cinco anos.

Published

2021

7. Leukotriene A4 Hydrolase (LTA4H) is expressed in leprosy lesions and variants are associated with susceptibility to mycobacterial diseases

Author

Vary, JC, Tobin, DM, Dunstan, SJ, Bang, ND, Hagge, DA, Khadge, S, King, M, Ramakrishnan, L, and Hawn, TR

Published

2016

8. The Many Hosts of Mycobacteria 9 (MHM9): A conference report.

Author

Klever AM, Alexander KA, Almeida D, Anderson MZ, Ball RL, Beamer G, Boggiatto P, Buikstra JE, Chandler B, Claeys TA, Concha AE, Converse PJ, Derbyshire KM, Dobos KM, Dupnik KM, Endsley JJ, Endsley MA, Fennelly K, Franco-Paredes C, Hagge DA, Hall-Stoodley L, Hayes D Jr, Hirschfeld K, Hofman CA, Honda JR, Hull NM, Kramnik I, Lacourciere K, Lahiri R, Lamont EA, Larsen MH, Lemaire T, Lesellier S, Lee NR, Lowry CA, Mahfooz NS, McMichael TM, Merling MR, Miller MA, Nagajyothi JF, Nelson E, Nuermberger EL, Pena MT, Perea C, Podell BK, Pyle CJ, Quinn FD, Rajaram MVS, Mejia OR, Rothoff M, Sago SA, Salvador LCM, Simonson AW, Spencer JS, Sreevatsan S, Subbian S, Sunstrum J, Tobin DM, Vijayan KKV, Wright CTO, and Robinson RT

Subjects

Animals, Cattle, Humans, Nontuberculous Mycobacteria, Coinfection, Mycobacterium Infections, Nontuberculous microbiology, Mycobacterium tuberculosis, Tuberculosis, Bovine

Abstract

The Many Hosts of Mycobacteria (MHM) meeting series brings together basic scientists, clinicians and veterinarians to promote robust discussion and dissemination of recent advances in our knowledge of numerous mycobacterial diseases, including human and bovine tuberculosis (TB), nontuberculous mycobacteria (NTM) infection, Hansen's disease (leprosy), Buruli ulcer and Johne's disease. The 9th MHM conference (MHM9) was held in July 2022 at The Ohio State University (OSU) and centered around the theme of "Confounders of Mycobacterial Disease." Confounders can and often do drive the transmission of mycobacterial diseases, as well as impact surveillance and treatment outcomes. Various confounders were presented and discussed at MHM9 including those that originate from the host (comorbidities and coinfections) as well as those arising from the environment (e.g., zoonotic exposures), economic inequality (e.g. healthcare disparities), stigma (a confounder of leprosy and TB for millennia), and historical neglect (a confounder in Native American Nations). This conference report summarizes select talks given at MHM9 highlighting recent research advances, as well as talks regarding the historic and ongoing impact of TB and other infectious diseases on Native American Nations, including those in Southwestern Alaska where the regional TB incidence rate is among the highest in the Western hemisphere., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

9. A Sensitive and Quantitative Assay to Enumerate and Measure Mycobacterium leprae Viability in Clinical and Experimental Specimens.

Author

Collins JH, Lenz SM, Ray NA, Balagon MF, Hagge DA, Lahiri R, and Adams LB

Subjects

DNA, Bacterial genetics, Humans, RNA, Bacterial genetics, Real-Time Polymerase Chain Reaction, Leprosy diagnosis, Mycobacterium leprae genetics

Abstract

Mycobacterium leprae, the etiologic agent of leprosy, cannot be cultured on artificial media. This characteristic, coupled with its long generation time, presents a number of unique challenges to studying this pathogen. One of the difficulties facing both researchers and clinicians is the absence of a rapid test to measure the viability of M. leprae in clinical or experimental specimens. The lack of such a tool limits the understanding of M. leprae immunopathogenesis and makes determining the efficacy of drug treatments difficult. With this in mind, we developed a robust two-step molecular viability assay (MVA) that first enumerates the M. leprae in the tissue; then, this data is used to normalize bacterial RNA quantities for the second step, in which the expression of M. leprae esxA and hsp18 are measured. This assay is specific and sensitive enough to be used on most clinical samples. This protocol describes the steps required to extract DNA and RNA from M. leprae-infected tissue, enumerate M. leprae, and measure M. leprae viability based on the normalized expression of two M. leprae-specific genes (hsp18 and esxA). This protocol also outlines an optimal laboratory design and workflow for performing this assay. © 2022 The Leprosy Mission Nepal. Current Protocols published by Wiley Periodicals LLC. This article has been contributed to by US Government employees and their work is in the public domain in the USA. Basic Protocol 1: DNA and RNA P purification from M. leprae-infected tissue Basic Protocol 2: Enumeration of M. leprae by RLEP qPCR on the DNA fraction Basic Protocol 3: Calculation of M. leprae per tissue and normalization of RNA Basic Protocol 4: Reverse-transcription of normalized RNA to generate cDNA Basic Protocol 5: Determination of M. leprae viability using HSP18 and ESXA qPCR on the cDNA Support Protocol 1: M. leprae qPCR primer/probe stock preparation Support Protocol 2: Preparation of plasmid stocks and standard curves., (© 2022 The Leprosy Mission Nepal. Current Protocols published by Wiley Periodicals LLC. This article has been contributed to by US Government employees and their work is in the public domain in the USA.)

Published

2022

10. Correction: A Sensitive and Quantitative Assay to Enumerate and Measure Mycobacterium leprae Viability in Clinical and Experimental Specimens.

Author

Collins JH, Lenz SM, Ray NA, Balagon MF, Hagge DA, Lahiri R, and Adams LB

Published

2022

11. A simple assay to quantify mycobacterial lipid antigen-specific T cell receptors in human tissues and blood.

Author

Zhou AX, Scriba TJ, Day CL, Hagge DA, and Seshadri C

Subjects

Antigens, CD1 genetics, Antigens, CD1 immunology, Cell Wall genetics, Cell Wall immunology, Cohort Studies, Humans, Leprosy blood, Leprosy immunology, Leprosy microbiology, Mycobacterium genetics, Mycobacterium isolation & purification, Nepal, Polymerase Chain Reaction, Receptors, Antigen, T-Cell, alpha-beta blood, Receptors, Antigen, T-Cell, alpha-beta genetics, South Africa, T-Lymphocytes immunology, T-Lymphocytes microbiology, Tuberculosis blood, Tuberculosis immunology, Tuberculosis microbiology, Leprosy diagnosis, Lipids immunology, Molecular Diagnostic Techniques methods, Mycobacterium immunology, Receptors, Antigen, T-Cell, alpha-beta immunology, Tuberculosis diagnosis

Abstract

T cell receptors (TCRs) encode the history of antigenic challenge within an individual and have the potential to serve as molecular markers of infection. In addition to peptide antigens bound to highly polymorphic MHC molecules, T cells have also evolved to recognize bacterial lipids when bound to non-polymorphic CD1 molecules. One such subset, germline-encoded, mycolyl lipid-reactive (GEM) T cells, recognizes mycobacterial cell wall lipids and expresses a conserved TCR-ɑ chain that is shared among genetically unrelated individuals. We developed a quantitative PCR assay to determine expression of the GEM TCR-ɑ nucleotide sequence in human tissues and blood. This assay was validated on plasmids and T cell lines. We tested blood samples from South African subjects with or without tuberculin reactivity or with active tuberculosis disease. We were able to detect GEM TCR-ɑ above the limit of detection in 92% of donors but found no difference in GEM TCR-ɑ expression among the three groups after normalizing for total TCR-ɑ expression. In a cohort of leprosy patients from Nepal, we successfully detected GEM TCR-ɑ in 100% of skin biopsies with histologically confirmed tuberculoid and lepromatous leprosy. Thus, GEM T cells constitute part of the T cell repertoire in the skin. However, GEM TCR-ɑ expression was not different between leprosy patients and control subjects after normalization. Further, these results reveal the feasibility of developing a simple, field deployable molecular diagnostic based on mycobacterial lipid antigen-specific TCR sequences that are readily detectable in human tissues and blood independent of genetic background., Competing Interests: The authors have declared that no competing interests exist.

Published

2021

12. An assessment of the reported impact of the COVID-19 pandemic on leprosy services using an online survey of practitioners in leprosy referral centres.

Author

de Barros B, Lambert SM, Negera E, de Arquer GR, Sales AM, Darlong J, Dias VLA, Rozario BJ, Pai VV, Alinda MD, Listiawan MY, Hagge DA, Shah M, Lockwood DNJ, and Walker SL

Subjects

Cross-Sectional Studies, Drug Therapy, Combination, Humans, Leprostatic Agents, Pandemics prevention & control, Referral and Consultation, SARS-CoV-2, Surveys and Questionnaires, COVID-19, Leprosy diagnosis, Leprosy drug therapy, Leprosy epidemiology

Abstract

Background: The coronavirus disease 2019 (COVID-19) pandemic has led to governments implementing a variety of public health measures to control transmission and has affected health services. Leprosy is a communicable neglected tropical disease caused by Mycobacterium leprae and is an important health problem in low- and middle-income countries. The natural history of leprosy means that affected individuals need long-term follow-up. The measures recommended to reduce transmission of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) can create barriers to health services. We evaluated the impact of the COVID-19 epidemic response on leprosy services and disease management., Methods: We conducted a cross-sectional online survey with healthcare professionals in leprosy referral centres., Results: Eighty percent of leprosy diagnostic services were reduced. All respondents reported that multidrug therapy (MDT) was available but two reported a reduced stock. Clinicians used alternative strategies such as telephone consultations to maintain contact with patients. However, patients were not able to travel to the referral centres., Discussion: This study highlights the effects of the initial phase of the SARS-CoV-2 pandemic on leprosy services in a range of leprosy-endemic countries. Many services remained open, providing leprosy diagnosis, MDT and leprosy reaction medications. Centres developed innovative measures to counter the negative impacts of the COVID-19 pandemic., (© The Author(s) 2021. Published by Oxford University Press on behalf of Royal Society of Tropical Medicine and Hygiene.)

Published

2021

13. An individual randomised efficacy trial of autologous blood products, leukocyte and platelet-rich fibrin (L-PRF), to promote ulcer healing in leprosy in Nepal: the TABLE trial protocol.

Author

Napit IB, Shrestha D, Bishop J, Choudhury S, Dulal S, Gill P, Gkini E, Gwyther H, Hagge DA, Neupane K, Sartori J, Slinn G, Watson SI, and Lilford R

Subjects

Adolescent, Adult, Drug Therapy, Combination, Humans, Leprostatic Agents, Leukocytes, Nepal, Quality of Life, Randomized Controlled Trials as Topic, Ulcer, Leprosy diagnosis, Leprosy therapy, Platelet-Rich Fibrin

Abstract

Background: Leprosy is curable with multidrug therapy and treatment in the early stages can prevent disability. However, local nerve damage can lead to injury and consequently recurring and disfiguring ulcers. The aim of this study is to evaluate the treatment of leprosy ulcers using an autologous blood product; leukocyte and platelet-rich fibrin (L-PRF) to promote healing., Methods: This is a single-centre study in the Anandaban Hospital, The Leprosy Mission Nepal, Kathmandu, Nepal. Consenting patients (n=130) will be individually randomised in a single-blinded, controlled trial. Participants will be 18 years of age or older, admitted to the hospital with a clean, dry and infection-free chronic foot ulcer between 2 and 20 cm 2 in size. If the ulcer is infected, it will be treated before enrolment into the study. The intervention involves the application of leukocyte and platelet-rich fibrin (L-PRF) matrix on the ulcer beds during twice-weekly dressing changes. Controls receive usual care in the form of saline dressings only during their twice-weekly dressing changes. Primary outcomes are the rate of healing assessed using standardised photographs by observers blind to allocated treatment, and time to complete re-epithelialization. Follow-up is at 6 months from randomisation., Discussion: This research will provide valuable information on the clinical and cost-effectiveness of L-PRF in the treatment of leprosy ulcers. An additional benefit is the evaluation of the effects of treatment on quality of life for people living with leprosy ulcers. The results will improve our understanding of the scalability of this treatment across low-income countries for ulcer healing in leprosy and potentially other conditions such as diabetic ulcers., Trial Registration: ClinicalTrials.gov ISRCTN14933421 . Registered on 16 June 2020., (© 2021. The Author(s).)

Published

2021

14. Methotrexate and prednisolone study in erythema nodosum leprosum (MaPs in ENL) protocol: a double-blind randomised clinical trial.

Author

de Barros B, Lambert SM, Shah M, Pai VV, Darlong J, Rozario BJ, Alinda MD, Sales AM, Doni S, Hagge DA, Shrestha D, Listiawan MY, Yitaye AM, Nery JAC, Neupane KD, Dias VLA, Butlin CR, Nicholls PG, Lockwood D, and Walker SL

Subjects

Bangladesh, Brazil, Ethiopia, Humans, India, Indonesia, Leprostatic Agents therapeutic use, London, Nepal, Erythema Nodosum drug therapy, Leprosy, Lepromatous drug therapy, Methotrexate therapeutic use, Prednisolone therapeutic use

Abstract

Introduction: Erythema nodosum leprosum (ENL) is an immunological complication of leprosy. ENL results in morbidity and disability and if it is not treated can lead to death. The current treatment consists of thalidomide or high doses of oral corticosteroids for prolonged periods. Thalidomide is not available in many leprosy endemic countries. The use of corticosteroids is associated with morbidity and mortality. Identifying treatment regimens that reduce the use of corticosteroids in ENL is essential. Methotrexate (MTX) is used to treat many inflammatory diseases and has been used successfully to treat patients with ENL not controlled by other drugs, including prednisolone and thalidomide. We present the protocol of the 'MTX and prednisolone study in ENL' (MaPs in ENL) a randomised controlled trial (RCT) designed to test the efficacy of MTX in the management of ENL., Methods and Analysis: MaPs in ENL is an international multicentre RCT, which will be conducted in leprosy referral centres in Bangladesh, Brazil, Ethiopia, India, Indonesia and Nepal. Patients diagnosed with ENL who consent to participate will be randomly allocated to receive 48 weeks of weekly oral MTX plus 20 weeks of prednisolone or 48 weeks of placebo plus 20 weeks of prednisolone. Participants will be stratified by type of ENL into those with acute ENL and those with chronic and recurrent ENL. The primary objective is to determine whether MTX reduces the requirement for additional prednisolone. Patients' reported outcome measures will be used to assess the efficacy of MTX. Participants will be closely monitored for adverse events., Ethics and Dissemination: Results will be submitted for publication in peer-reviewed journals. Ethical approval was obtained from the Observational/Interventions Research Ethics Committee of the London School of Hygiene & Tropical Medicine (15762); The Leprosy Mission International Bangladesh Institutional Research Board (in process); AHRI-ALERT Ethical Review Committee, Ethiopia; Ethics Committee of the Managing Committee of the Bombay Leprosy Project; and The Leprosy Mission Trust India Ethics Committee; the Nepal Health and Research Council and Health Research Ethics Committee Dr. Soetomo, Indonesia. This study is registered at www.clinicaltrials.gov. This is the first RCT of MTX for ENL and will contribute to the evidence for the management of ENL.Trial registration numberNCT 03775460., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

15. Post-exposure prophylaxis (PEP) efficacy of rifampin, rifapentine, moxifloxacin, minocycline, and clarithromycin in a susceptible-subclinical model of leprosy.

Author

Lenz SM, Collins JH, Ray NA, Hagge DA, Lahiri R, and Adams LB

Subjects

Animals, Bacterial Load drug effects, Clarithromycin therapeutic use, Drug Combinations, Leprosy transmission, Mice, Mice, Nude, Minocycline therapeutic use, Moxifloxacin therapeutic use, Mycobacterium leprae growth & development, Rifampin analogs & derivatives, Rifampin therapeutic use, Asymptomatic Infections therapy, Leprostatic Agents therapeutic use, Leprosy drug therapy, Mycobacterium leprae drug effects, Post-Exposure Prophylaxis methods

Abstract

Background: Subclinical infection with Mycobacterium leprae is one potential source of leprosy transmission, and post-exposure prophylaxis (PEP) regimens have been proposed to control this source. Because PEP trials require considerable investment, we applied a sensitive variation of the kinetic mouse footpad (MFP) screening assay to aid in the choice of drugs and regimens for clinical trials., Methodology/principal Findings: Athymic nude mice were inoculated in the footpad (FP) with 6 x 103 viable M. leprae and treated by gastric gavage with a single dose of Rifampin (SDR), Rifampin + Ofloxacin + Minocycline (SD-ROM), or Rifapentine + Minocycline + Moxifloxacin (SD-PMM) or with the proposed PEP++ regimen of three once-monthly doses of Rifampin + Moxifloxacin (RM), Rifampin + Clarithromycin (RC), Rifapentine + Moxifloxacin (PM), or Rifapentine + Clarithromycin (PC). At various times post-treatment, DNA was purified from the FP, and M. leprae were enumerated by RLEP quantitative PCR. A regression analysis was calculated to determine the expected RLEP value if 99.9% of the bacilli were killed after the administration of each regimen. SDR and SD-ROM induced little growth delay in this highly susceptible murine model of subclinical infection. In contrast, SD-PMM delayed measurable M. leprae growth above the inoculum by 8 months. The four multi-dose regimens delayed bacterial growth for >9months post-treatment cessation., Conclusions/significance: The delay in discernable M. leprae growth post-treatment was an excellent indicator of drug efficacy for both early (3-4 months) and late (8-9 months) drug efficacy. Our data indicates that multi-dose PEP may be required to control infection in highly susceptible individuals with subclinical leprosy to prevent disease and decrease transmission., Competing Interests: The authors have declared that no competing interests exist.

Published

2020

16. Whole blood RNA signatures in leprosy patients identify reversal reactions before clinical onset: a prospective, multicenter study.

Author

Tió-Coma M, van Hooij A, Bobosha K, van der Ploeg-van Schip JJ, Banu S, Khadge S, Thapa P, Kunwar CB, Goulart IM, Bekele Y, Hagge DA, Moraes MO, Teles RMB, Pinheiro RO, van Zwet EW, Goeman JJ, Aseffa A, Haks MC, Ottenhoff THM, Modlin RL, and Geluk A

Subjects

Adolescent, Adult, Bangladesh epidemiology, Biomarkers blood, Brazil epidemiology, Ethiopia epidemiology, Female, Humans, Leprosy blood, Leprosy epidemiology, Male, Mycobacterium leprae isolation & purification, Nepal epidemiology, Netherlands epidemiology, Prognosis, Prospective Studies, Young Adult, Leprosy genetics, Transcriptome

Abstract

Early diagnosis of leprosy is challenging, particularly its inflammatory reactions, the major cause of irreversible neuropathy in leprosy. Current diagnostics cannot identify which patients are at risk of developing reactions. This study assessed blood RNA expression levels as potential biomarkers for leprosy. Prospective cohorts of newly diagnosed leprosy patients, including reactions, and healthy controls were recruited in Bangladesh, Brazil, Ethiopia and Nepal. RNA expression in 1,090 whole blood samples was determined for 103 target genes for innate and adaptive immune profiling by dual color Reverse-Transcription Multiplex Ligation-dependent Probe Amplification (dcRT-MLPA) followed by cluster analysis. We identified transcriptomic biomarkers associated with leprosy disease, different leprosy phenotypes as well as high exposure to Mycobacterium leprae which respectively allow improved diagnosis and classification of leprosy patients and detection of infection. Importantly, a transcriptomic signature of risk for reversal reactions consisting of five genes (CCL2, CD8A, IL2, IL15 and MARCO) was identified based on cross-sectional comparison of RNA expression. In addition, intra-individual longitudinal analyses of leprosy patients before, during and after treatment of reversal reactions, indicated that several IFN-induced genes increased significantly at onset of reaction whereas IL15 decreased. This multi-site study, situated in four leprosy endemic areas, demonstrates the potential of host transcriptomic biomarkers as correlates of risk for leprosy. Importantly, a prospective five-gene signature for reversal reactions could predict reversal reactions at least 2 weeks before onset. Thus, transcriptomic biomarkers provide promise for early detection of these acute inflammatory episodes and thereby help prevent permanent neuropathy and disability in leprosy patients.

Published

2019

17. Diagnosis and impact of neuropathic pain in leprosy patients in Nepal after completion of multidrug therapy.

Author

Toh HS, Maharjan J, Thapa R, Neupane KD, Shah M, Baral S, Hagge DA, Napit IB, and Lockwood DNJ

Subjects

Adult, Aged, Cross-Sectional Studies, Drug Therapy, Combination, Female, Humans, Leprosy diagnosis, Leprosy drug therapy, Male, Middle Aged, Nepal epidemiology, Neuralgia epidemiology, Neuralgia psychology, Quality of Life, Surveys and Questionnaires, Young Adult, Leprostatic Agents administration & dosage, Leprosy complications, Neuralgia etiology

Abstract

Objectives: Neuropathic pain (NP) can occur as a chronic complication of leprosy neuropathy. NP epidemiology and its impact on patients have not been well documented. This study investigates NP prevalence and impact in the years after patients are declared "released from treatment" (RFT) following multidrug therapy (MDT) completion., Methods: In this cross-sectional study, 85 RFT patients were recruited within leprosy referral services in Nepal. The Douleur Neuropathique 4 Questionnaire (DN4) was used to screen for NP. Pain severity, impacts on patients' daily activities and mental health were measured by using the Brief Pain Inventory (BPI), Screening of Activity Limitation and Safety Awareness (SALSA), and General Health Questionnaire-12 (GHQ-12) respectively., Results: 96% surveyed had been treated for multibacillary leprosy. 44 (52%) complained of pain of which 30 (68%) were diagnosed with NP. NP was not associated with age, gender, or presence of skin lesions or nerve symptoms at leprosy diagnosis. 70% of patients with NP had either history of or ongoing reactions and 47% had grade 2 disability. Nerve tenderness (p = 0.023) and current reactions (p = 0.018) were significant risk factors for NP. Patients with NP suffered significantly higher intensity pain (p = 0.023) and daily life interference (p = 0.003) and were more likely to have moderate to extreme daily activity limitations (p = 0.005). 13 (43%) exhibited psychological distress, and medications only reduced moderate degree (50-60%) of pain., Conclusions: In our study, 35% of RFT patients had ongoing NP. Risk factors include nerve tenderness and reaction. They suffer from more daily life interference and psychological distress. Leprosy patient care should include recognition and management of NP., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

18. Opening a Can of Worms: Leprosy Reactions and Complicit Soil-Transmitted Helminths.

Author

Hagge DA, Parajuli P, Kunwar CB, Rana DRSJB, Thapa R, Neupane KD, Nicholls P, Adams LB, Geluk A, Shah M, and Napit IB

Subjects

Female, Global Health, Helminthiasis diagnosis, Helminthiasis immunology, Helminthiasis transmission, Humans, Leprosy immunology, Male, Prevalence, Coinfection, Disease Susceptibility, Helminthiasis epidemiology, Host-Parasite Interactions immunology, Leprosy epidemiology, Soil parasitology

Abstract

Background: >94% of new annual leprosy cases are diagnosed in populations co-endemic for soil-transmitted helminths (STH). STH can profoundly dysregulate host immune responses towards Th2 bias, which can be restored over time after deworming. We hypothesize that STH co-infection is associated with leprosy reaction (denoted as simply "reaction" herein) occurrence within a co-endemic population., Methods: A cohort study was performed on a cohort of Nepalese leprosy patients across treatment and diagnostic classifications who were screened by routine fecal smear microscopy and multiplex quantitative PCR (qPCR) for Ascaris lumbricoides (Al), Strongyloides stercoralis (Ss), Ancyclostoma duodenale (Ad) and Necator americanus (Na)., Results: Among 145 patients, 55% were positive for ≥1 STH (STH+): 34% Al+, 18% Ss+, 17% Ad+and 5% Na+. Significant inverse STH and reaction relationships were evidenced by the bulk of cases: 63% reaction-negative were STH+ of total cases (p=0.030) while 65% reaction-positive were STH- in new cases (96; p=0.023). Strikingly, the majority of STH+ were reaction-negative, even when considering each species: 59% Al+, 60% Ss+, 62% Ad+and 67% Na+of new leprosy cases., Conclusions: Absence of STH co-infection is associated with leprosy reaction at diagnosis within a co-endemic population. This is likely due to immune reconstitution effects after deworming or interruption of chronic STH-mediated immune dysregulation., (Copyright © 2017. Published by Elsevier B.V.)

Published

2017

19. A leprosy clinical severity scale for erythema nodosum leprosum: An international, multicentre validation study of the ENLIST ENL Severity Scale.

Author

Walker SL, Sales AM, Butlin CR, Shah M, Maghanoy A, Lambert SM, Darlong J, Rozario BJ, Pai VV, Balagon M, Doni SN, Hagge DA, Nery JAC, Neupane KD, Baral S, Sangma BA, Alembo DT, Yetaye AM, Hassan BA, Shelemo MB, Nicholls PG, and Lockwood DNJ

Subjects

Adult, Female, Humans, Male, Middle Aged, Young Adult, Erythema Nodosum pathology, Leprosy, Lepromatous pathology, Severity of Illness Index

Abstract

Objectives: We wished to validate our recently devised 16-item ENLIST ENL Severity Scale, a clinical tool for measuring the severity of the serious leprosy associated complication of erythema nodosum leprosum (ENL). We also wished to assess the responsiveness of the ENLIST ENL Severity Scale in detecting clinical change in patients with ENL., Methods: Participants, recruited from seven centres in six leprosy endemic countries, were assessed using the ENLIST ENL Severity Scale by two researchers, one of whom categorised the severity of ENL. At a subsequent visit a further assessment using the scale was made and both participant and physician rated the change in ENL using the subjective categories of "Much better", "somewhat better", "somewhat worse" and "much worse" compared with "No change" or "about the same"., Results: 447 participants were assessed with the ENLIST ENL Severity Scale. The Cronbach alpha of the scale and each item was calculated to determine the internal consistency of the scale. The ENLIST ENL Severity Scale had good internal consistency and this improved following removal of six items to give a Cronbach's alpha of 0.77. The cut off between mild ENL and more severe disease was 9 determined using ROC curves. The minimal important difference of the scale was determined to be 5 using both participant and physician ratings of change., Conclusions: The 10-item ENLIST ENL Severity Scale is the first valid, reliable and responsive measure of ENL severity and improves our ability to assess and compare patients and their treatments in this severe and difficult to manage complication of leprosy. The ENLIST ENL Severity Scale will assist physicians in the monitoring and treatment of patients with ENL. The ENLIST ENL Severity Scale is easy to apply and will be useful as an outcome measure in treatment studies and enable the standardisation of other clinical and laboratory ENL research.

Published

2017

20. Genetic Variation in Toll-Interacting Protein Is Associated With Leprosy Susceptibility and Cutaneous Expression of Interleukin 1 Receptor Antagonist.

Author

Shah JA, Berrington WR, Vary JC Jr, Wells RD, Peterson GJ, Kunwar CB, Khadge S, Hagge DA, and Hawn TR

Subjects

Adult, Case-Control Studies, Genotype, Humans, Interleukin 1 Receptor Antagonist Protein genetics, Intracellular Signaling Peptides and Proteins genetics, Leprosy epidemiology, Nepal, Prospective Studies, Skin metabolism, Gene Expression Regulation, Bacterial physiology, Genetic Predisposition to Disease, Interleukin 1 Receptor Antagonist Protein metabolism, Intracellular Signaling Peptides and Proteins metabolism, Leprosy genetics, Polymorphism, Single Nucleotide

Abstract

Leprosy is a chronic disease characterized by skin and peripheral nerve pathology and immune responses that fail to control Mycobacterium leprae. Toll-interacting protein (TOLLIP) regulates Toll-like receptor (TLR) and interleukin 1 receptor (IL-1R) signaling against mycobacteria. We analyzed messenger RNA (mRNA) expression of candidate immune genes in skin biopsy specimens from 85 individuals with leprosy. TOLLIP mRNA was highly and specifically correlated with IL-1R antagonist (IL-1Ra). In a case-control gene-association study with 477 cases and 1021 controls in Nepal, TOLLIP single-nucleotide polymorphism rs3793964 TT genotype was associated with increased susceptibility to leprosy (recessive, P = 1.4 × 10(-3)) and with increased skin expression of TOLLIP and IL-1Ra. Stimulation of TOLLIP-deficient monocytes with M. leprae produced significantly less IL-1Ra (P < .001), compared with control. These data suggest that M. leprae upregulates IL-1Ra by a TOLLIP-dependent mechanism. Inhibition of TOLLIP may decrease an individual's susceptibility to leprosy and offer a novel therapeutic target for IL-1-dependent diseases., (© The Author 2015. Published by Oxford University Press for the Infectious Diseases Society of America. All rights reserved. For permissions, e-mail journals.permissions@oup.com.)

Published

2016

21. Exploratory urinary metabolomics of type 1 leprosy reactions.

Author

Mayboroda OA, van Hooij A, Derks R, van den Eeden SJ, Dijkman K, Khadge S, Thapa P, Kunwar CB, Hagge DA, and Geluk A

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Biomarkers urine, Cohort Studies, Female, Humans, Leprosy diagnosis, Male, Middle Aged, Prospective Studies, Leprosy urine, Metabolomics

Abstract

Background: Leprosy is an infectious disease caused by Mycobacterium leprae that affects the skin and nerves. Although curable with multidrug therapy, leprosy is complicated by acute inflammatory episodes called reactions, which are the major causes of irreversible neuropathy in leprosy that occur before, during, and even after treatment. Early diagnosis and prompt treatment of reactions reduces the risk of permanent disability., Methods: This exploratory study investigated whether urinary metabolic profiles could be identified that correlate with early signs of reversal reactions (RR). A prospective cohort of leprosy patients with and without reactions and endemic controls was recruited in Nepal. Urine-derived metabolic profiles were measured longitudinally. Thus, a conventional area of biomarker identification for leprosy was extended to non-invasive urine testing., Results: It was found that the urinary metabolome could be used to discriminate endemic controls from untreated patients with mycobacterial disease. Moreover, metabolic signatures in the urine of patients developing RR were clearly different before RR onset compared to those at RR diagnosis., Conclusions: This study indicates that urinary metabolic profiles are promising host biomarkers for the detection of intra-individual changes during acute inflammation in leprosy and could contribute to early treatment and prevention of tissue damage., (Copyright © 2016 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2016

22. Persistent dengue emergence: the 7 years surrounding the 2010 epidemic in Nepal.

Author

Pandey BD, Pandey K, Neupane B, Shah Y, Adhikary KP, Gautam I, Hagge DA, and Morita K

Subjects

Adolescent, Adult, Age Distribution, Dengue Virus immunology, Enzyme-Linked Immunosorbent Assay, Female, Humans, Immunoglobulin M blood, Male, Middle Aged, Nepal epidemiology, Prevalence, Seasons, Seroepidemiologic Studies, Sex Distribution, Young Adult, Dengue epidemiology

Abstract

Background: Dengue fever (DF) is an emerging public health problem in Nepal, and yet neither the magnitude of the DF burden or its epidemiological trends are well understood., Methods: We conducted a sero-epidemiological, seasonal trend and demographic analysis of the trends in DF in the Terai region of Nepal, from 2007 to 2013. In that period, 2002 serum samples were collected from febrile patients suspected of dengue virus infection. Samples were screened by IgM antibody ELISA analysis for the presence of anti-dengue IgM antibodies., Results: The overall prevalence of DF cases was found to range from 26.1 to 55.4%. Infection was found to be more common among adults and males. Seasonal trends revealed that cases peaked in October and November., Conclusions: The study offers perspective on the dengue fever burden before, during and after a major epidemic and can now be used as a basis for formulating strategies by policy makers that will enhance and develop relevant control and preventive measures against dengue fever. The findings of this study reinforce the perceived need for urgent dengue virus surveillance to enhance dengue control strategies that need to be developed for future preparedness. In the light of the recent earthquakes, future major outbreaks of vector borne disease are likely to recur., (© The Author 2015. Published by Oxford University Press on behalf of Royal Society of Tropical Medicine and Hygiene. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2015

23. Longitudinal immune profiles in type 1 leprosy reactions in Bangladesh, Brazil, Ethiopia and Nepal.

Author

Khadge S, Banu S, Bobosha K, van der Ploeg-van Schip JJ, Goulart IM, Thapa P, Kunwar CB, van Meijgaarden KE, van den Eeden SJ, Wilson L, Kabir S, Dey H, Goulart LR, Lobato J, Carvalho W, Bekele Y, Franken KL, Aseffa A, Spencer JS, Oskam L, Otttenhoff TH, Hagge DA, and Geluk A

Subjects

Bangladesh, Brazil, Cytokines blood, Ethiopia, Female, Host-Pathogen Interactions, Humans, Immunity, Humoral immunology, Interleukin-10 blood, Interleukin-17 blood, Leprosy diagnosis, Leukocytes, Mononuclear immunology, Leukocytes, Mononuclear microbiology, Male, Middle Aged, Mycobacterium leprae immunology, Nepal, Prospective Studies, Biomarkers analysis, Cytokines immunology, Leprosy immunology, Mycobacterium leprae pathogenicity

Abstract

Background: Acute inflammatory reactions are a frequently occurring, tissue destructing phenomenon in infectious- as well as autoimmune diseases, providing clinical challenges for early diagnosis. In leprosy, an infectious disease initiated by Mycobacterium leprae (M. leprae), these reactions represent the major cause of permanent neuropathy. However, laboratory tests for early diagnosis of reactional episodes which would significantly contribute to prevention of tissue damage are not yet available. Although classical diagnostics involve a variety of tests, current research utilizes limited approaches for biomarker identification. In this study, we therefore studied leprosy as a model to identify biomarkers specific for inflammatory reactional episodes., Methods: To identify host biomarker profiles associated with early onset of type 1 leprosy reactions, prospective cohorts including leprosy patients with and without reactions were recruited in Bangladesh, Brazil, Ethiopia and Nepal. The presence of multiple cyto-/chemokines induced by M. leprae antigen stimulation of peripheral blood mononuclear cells as well as the levels of antibodies directed against M. leprae-specific antigens in sera, were measured longitudinally in patients., Results: At all sites, longitudinal analyses showed that IFN-γ-, IP-10-, IL-17- and VEGF-production by M. leprae (antigen)-stimulated PBMC peaked at diagnosis of type 1 reactions, compared to when reactions were absent. In contrast, IL-10 production decreased during type 1 reaction while increasing after treatment. Thus, ratios of these pro-inflammatory cytokines versus IL-10 provide useful tools for early diagnosing type 1 reactions and evaluating treatment. Of further importance for rapid diagnosis, circulating IP-10 in sera were significantly increased during type 1 reactions. On the other hand, humoral immunity, characterized by M. leprae-specific antibody detection, did not identify onset of type 1 reactions, but allowed treatment monitoring instead., Conclusions: This study identifies immune-profiles as promising host biomarkers for detecting intra-individual changes during acute inflammation in leprosy, also providing an approach for other chronic (infectious) diseases to help early diagnose these episodes and contribute to timely treatment and prevention of tissue damage.

Published

2015

24. ENLIST 1: An International Multi-centre Cross-sectional Study of the Clinical Features of Erythema Nodosum Leprosum.

Author

Walker SL, Balagon M, Darlong J, Doni SN, Hagge DA, Halwai V, John A, Lambert SM, Maghanoy A, Nery JA, Neupane KD, Nicholls PG, Pai VV, Parajuli P, Sales AM, Sarno E, Shah M, Tsegaye D, and Lockwood DN

Subjects

Adolescent, Adult, Aged, Child, Cross-Sectional Studies, Erythema Nodosum complications, Erythema Nodosum drug therapy, Female, Humans, International Cooperation, Leprostatic Agents therapeutic use, Male, Middle Aged, Pain physiopathology, Young Adult, Erythema Nodosum pathology, Leprosy, Lepromatous complications, Severity of Illness Index

Abstract

Erythema nodosum leprosum (ENL) is a severe multisystem immune mediated complication of borderline lepromatous leprosy and lepromatous leprosy. ENL is associated with skin lesions, neuritis, arthritis, dactylitis, eye inflammation, osteitis, orchitis, lymphadenitis and nephritis. The treatment of ENL requires immunosuppression, which is often required for prolonged periods of time and may lead to serious adverse effects. ENL and its treatment is associated with increased mortality and economic hardship. Improved, evidence-based treatments for ENL are needed; however, defining the severity of ENL and outcome measures for treatment studies is difficult because of the multiple organ systems involved. A cross-sectional study was performed, by the members of the Erythema Nodosum Leprosum International STudy (ENLIST) Group, of patients with ENL attending seven leprosy referral centres in Brazil, Ethiopia, India, Nepal, the Philippines and the United Kingdom. We systematically documented the clinical features and type of ENL, its severity and the drugs used to treat it. Patients with chronic ENL were more likely to be assessed as having severe ENL. Pain, the most frequent symptom, assessed using a semi-quantitative scale was significantly worse in individuals with "severe" ENL. Our findings will determine the items to be included in a severity scale of ENL which we are developing and validating. The study also provides data on the clinical features of ENL, which can be incorporated into a definition of ENL and used for outcome measures in treatment studies.

Published

2015

25. Differential dermal expression of CCL17 and CCL18 in tuberculoid and lepromatous leprosy.

Author

Berrington WR, Kunwar CB, Neupane K, van den Eeden SJ, Vary JC Jr, Peterson GJ, Wells RD, Geluk A, Hagge DA, and Hawn TR

Subjects

Adult, Biomarkers analysis, Chemokine CCL17 metabolism, Chemokines, CC metabolism, Cluster Analysis, Erythema Nodosum pathology, Female, Gene Expression Regulation, Bacterial, Humans, Interleukin-10 genetics, Interleukin-10 metabolism, Leprosy, Lepromatous pathology, Leprosy, Tuberculoid pathology, Macrophages immunology, Male, Middle Aged, Skin pathology, Young Adult, Chemokine CCL17 genetics, Chemokines, CC genetics, Erythema Nodosum immunology, Leprosy, Lepromatous immunology, Leprosy, Tuberculoid immunology

Abstract

Background: Leprosy is characterized by polar clinical, histologic and immunological presentations. Previous immunologic studies of leprosy polarity were limited by the repertoire of cytokines known at the time., Methodology: We used a candidate gene approach to measure mRNA levels in skin biopsies from leprosy lesions. mRNA from 24 chemokines and cytokines, and 6 immune cell type markers were measured from 85 Nepalese leprosy subjects. Selected findings were confirmed with immunohistochemistry., Principal Results: Expression of three soluble mediators (CCL18, CCL17 and IL-10) and one macrophage cell type marker (CD14) was significantly elevated in lepromatous (CCL18, IL-10 and CD14) or tuberculoid (CCL17) lesions. Higher CCL18 protein expression by immunohistochemistry and a trend in increased serum CCL18 in lepromatous lesions was observed. No cytokines were associated with erythema nodosum leprosum or Type I reversal reaction following multiple comparison correction. Hierarchical clustering suggested that CCL18 was correlated with cell markers CD209 and CD14, while neither CCL17 nor CCL18 were highly correlated with classical TH1 and TH2 cytokines., Conclusions: Our findings suggest that CCL17 and CCL18 dermal expression is associated with leprosy polarity.

Published

2014

26. IL-10 and NOS2 modulate antigen-specific reactivity and nerve infiltration by T cells in experimental leprosy.

Author

Hagge DA, Scollard DM, Ray NA, Marks VT, Deming AT, Spencer JS, and Adams LB

Subjects

Animals, Disease Models, Animal, Female, Interleukin-10 genetics, Mice, Mice, Knockout, Nitric Oxide Synthase Type II genetics, Antigens, Bacterial immunology, CD4-Positive T-Lymphocytes immunology, Interleukin-10 immunology, Leprosy immunology, Mycobacterium leprae immunology, Nitric Oxide Synthase Type II immunology

Abstract

Background: Although immunopathology dictates clinical outcome in leprosy, the dynamics of early and chronic infection are poorly defined. In the tuberculoid region of the spectrum, Mycobacterium leprae growth is restricted yet a severe granulomatous lesion can occur. The evolution and maintenance of chronic inflammatory processes like those observed in the leprosy granuloma involve an ongoing network of communications via cytokines. IL-10 has immunosuppressive properties and IL-10 genetic variants have been associated with leprosy development and reactions., Methodology/principal Findings: The role of IL-10 in resistance and inflammation in leprosy was investigated using Mycobacterium leprae infection of mice deficient in IL-10 (IL-10-/-), as well as mice deficient in both inducible nitric oxide synthase (NOS2-/-) and IL-10 (10NOS2-/-). Although a lack of IL-10 did not affect M. leprae multiplication in the footpads (FP), inflammation increased from C57Bl/6 (B6)

Published

2014

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

Author

Rivoire BL, Groathouse NA, TerLouw S, Neupane KD, Ranjit C, Sapkota BR, Khadge S, Kunwar CB, Macdonald M, Hawksworth R, Thapa MB, Hagge DA, Tibbals M, Smith C, Dube T, She D, Wolff M, Zhou E, Makhene M, Mason R, Sizemore C, and Brennan PJ

Subjects

Adolescent, Adult, Antigens, Bacterial administration & dosage, Antigens, Bacterial immunology, Double-Blind Method, Female, Humans, Leprosy immunology, Male, Middle Aged, Mycobacterium leprae immunology, Sensitivity and Specificity, Young Adult, Antigens, Bacterial adverse effects, Leprosy diagnosis, Skin Tests adverse effects, Skin Tests methods

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: ClinicalTrials.gov NCT01920750 (Phase I), NCT00128193 (Phase II).

Published

2014

28. T-cell regulation in lepromatous leprosy.

Author

Bobosha K, Wilson L, van Meijgaarden KE, Bekele Y, Zewdie M, van der Ploeg-van Schip JJ, Abebe M, Hussein J, Khadge S, Neupane KD, Hagge DA, Jordanova ES, Aseffa A, Ottenhoff TH, and Geluk A

Subjects

Biopsy, Humans, Immunohistochemistry, Immunophenotyping, Interferon-gamma metabolism, Leukocytes, Mononuclear immunology, Microscopy, Confocal, Skin pathology, T-Lymphocyte Subsets immunology, Leprosy, Lepromatous immunology, Mycobacterium leprae immunology, T-Lymphocytes immunology

Abstract

Regulatory T (Treg) cells are known for their role in maintaining self-tolerance and balancing immune reactions in autoimmune diseases and chronic infections. However, regulatory mechanisms can also lead to prolonged survival of pathogens in chronic infections like leprosy and tuberculosis (TB). Despite high humoral responses against Mycobacterium leprae (M. leprae), lepromatous leprosy (LL) patients have the characteristic inability to generate T helper 1 (Th1) responses against the bacterium. In this study, we investigated the unresponsiveness to M. leprae in peripheral blood mononuclear cells (PBMC) of LL patients by analysis of IFN-γ responses to M. leprae before and after depletion of CD25+ cells, by cell subsets analysis of PBMC and by immunohistochemistry of patients' skin lesions. Depletion of CD25+ cells from total PBMC identified two groups of LL patients: 7/18 (38.8%) gained in vitro responsiveness towards M. leprae after depletion of CD25+ cells, which was reversed to M. leprae-specific T-cell unresponsiveness by addition of autologous CD25+ cells. In contrast, 11/18 (61.1%) remained anergic in the absence of CD25+ T-cells. For both groups mitogen-induced IFN-γ was, however, not affected by depletion of CD25+ cells. In M. leprae responding healthy controls, treated lepromatous leprosy (LL) and borderline tuberculoid leprosy (BT) patients, depletion of CD25+ cells only slightly increased the IFN-γ response. Furthermore, cell subset analysis showed significantly higher (p = 0.02) numbers of FoxP3+ CD8+CD25+ T-cells in LL compared to BT patients, whereas confocal microscopy of skin biopsies revealed increased numbers of CD68+CD163+ as well as FoxP3+ cells in lesions of LL compared to tuberculoid and borderline tuberculoid leprosy (TT/BT) lesions. Thus, these data show that CD25+ Treg cells play a role in M. leprae-Th1 unresponsiveness in LL.

Published

2014

29. Insights from animal models on the immunogenetics of leprosy: a review.

Author

Adams LB, Pena MT, Sharma R, Hagge DA, Schurr E, and Truman RW

Subjects

Animals, Armadillos microbiology, Mice immunology, Animals, Genetically Modified, Armadillos genetics, Disease Models, Animal, Immunogenetic Phenomena immunology, Leprosy genetics, Leprosy immunology, Mice genetics, Mycobacterium leprae genetics, Mycobacterium leprae immunology

Abstract

A variety of host immunogenetic factors appear to influence both an individual's susceptibility to infection with Mycobacterium leprae and the pathologic course of the disease. Animal models can contribute to a better understanding of the role of immunogenetics in leprosy through comparative studies helping to confirm the significance of various identified traits and in deciphering the underlying mechanisms that may be involved in expression of different disease related phenotypes. Genetically engineered mice, with specific immune or biochemical pathway defects, are particularly useful for investigating granuloma formation and resistance to infection and are shedding new light on borderline areas of the leprosy spectrum which are clinically unstable and have a tendency toward immunological complications. Though armadillos are less developed in this regard, these animals are the only other natural hosts of M. leprae and they present a unique opportunity for comparative study of genetic markers and mechanisms associable with disease susceptibility or resistance, especially the neurological aspects of leprosy. In this paper, we review the recent contributions of genetically engineered mice and armadillos toward our understanding of the immunogenetics of leprosy.

Published

2012

30. Comparison of two rapid tests for anti-phenolic glycolipid-I serology in Brazil and Nepal.

Author

Stefani MM, Grassi AB, Sampaio LH, Sousa AL, Costa MB, Scheelbeek P, Neupane KD, Hagge DA, Macdonald M, Cho SN, Oskam L, and Bührer-Sékula S

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Brazil, Case-Control Studies, Child, Child, Preschool, Chromatography, Affinity methods, Female, Humans, Immunoassay methods, Leprosy immunology, Male, Middle Aged, Nepal, Predictive Value of Tests, Reagent Kits, Diagnostic, Sensitivity and Specificity, Young Adult, Antigens, Bacterial blood, Glycolipids blood, Immunoglobulin Isotypes blood, Leprosy diagnosis, Mycobacterium leprae immunology

Abstract

The diagnosis of leprosy continues to be based on clinical symptoms and early diagnosis and treatment are critical to preventing disability and transmission. Sensitive and specific laboratory tests are not available for diagnosing leprosy. Despite the limited applicability of anti-phenolic glycolipid-I (PGL-I) serology for diagnosis, it has been suggested as an additional tool to classify leprosy patients (LPs) for treatment purposes. Two formats of rapid tests to detect anti-PGL-I antibodies [ML immunochromatography assay (ICA) and ML Flow] were compared in different groups, multibacillary patients, paucibacillary patients, household contacts and healthy controls in Brazil and Nepal. High ML Flow intra-test concordance was observed and low to moderate agreement between the results of ML ICA and ML Flow tests on the serum of LPs was observed. LPs were "seroclassified" according to the results of these tests and the seroclassification was compared to other currently used classification systems: the World Health Organization operational classification, the bacilloscopic index and the Ridley-Jopling classification. When analysing the usefulness of these tests in the operational classification of PB and MB leprosy for treatment and follow-up purposes, the ML Flow test was the best point-of-care test for subjects in Nepal and despite the need for sample dilution, the ML ICA test yielded better performance among Brazilian subjects. Our results identified possible ways to improve the performance of both tests.

Published

2012

31. Mycobacterium leprae virulence-associated peptides are indicators of exposure to M. leprae in Brazil, Ethiopia and Nepal.

Author

Bobosha K, Tang ST, van der Ploeg-van Schip JJ, Bekele Y, Martins MV, Lund O, Franken KL, Khadge S, Pontes MA, Gonçalves Hde S, Hussien J, Thapa P, Kunwar CB, Hagge DA, Aseffa A, Pessolani MC, Pereira GM, Ottenhoff TH, and Geluk A

Subjects

Bacterial Proteins immunology, Brazil, Computational Biology, Epitope Mapping, Ethiopia, Humans, Mycobacterium leprae immunology, Mycobacterium leprae isolation & purification, Mycobacterium leprae virology, Nepal, Peptide Fragments immunology, Recombinant Proteins immunology, Cytokines immunology, Epitopes, T-Lymphocyte immunology, Mycobacterium leprae pathogenicity, Virulence immunology

Abstract

Silent transmission of Mycobacterium leprae, as evidenced by stable leprosy incidence rates in various countries, remains a health challenge despite the implementation of multidrug therapy worldwide. Therefore, the development of tools for the early diagnosis of M. leprae infection should be emphasised in leprosy research. As part of the continuing effort to identify antigens that have diagnostic potential, unique M. leprae peptides derived from predicted virulence-associated proteins (group IV.A) were identified using advanced genome pattern programs and bioinformatics. Based on human leukocyte antigen (HLA)-binding motifs, we selected 21 peptides that were predicted to be promiscuous HLA-class I T-cell epitopes and eight peptides that were predicted to be HLA-class II restricted T-cell epitopes for field-testing in Brazil, Ethiopia and Nepal. High levels of interferon (IFN)-γ were induced when peripheral blood mononuclear cells (PBMCs) from tuberculoid/borderline tuberculoid leprosy patients located in Brazil and Ethiopia were stimulated with the ML2055 p35 peptide. PBMCs that were isolated from healthy endemic controls living in areas with high leprosy prevalence (EChigh) in Ethiopia also responded to the ML2055 p35 peptide. The Brazilian EChigh group recognised the ML1358 p20 and ML1358 p24 peptides. None of the peptides were recognised by PBMCs from healthy controls living in non-endemic region. In Nepal, mixtures of these peptides induced the production of IFN-γ by the PBMCs of leprosy patients and EChigh. Therefore, the M. leprae virulence-associated peptides identified in this study may be useful for identifying exposure to M. leprae in population with differing HLA polymorphisms.

Published

2012

32. The effect of systemic corticosteroid therapy on the expression of toll-like receptor 2 and toll-like receptor 4 in the cutaneous lesions of leprosy Type 1 reactions.

Author

Walker SL, Roberts CH, Atkinson SE, Khadge S, Macdonald M, Neupane KD, Ranjit C, Sapkota BR, Dhakal S, Hawksworth RA, Mahat K, Ruchal S, Hamal S, Hagge DA, and Lockwood DN

Subjects

Adolescent, Adult, Analysis of Variance, Antibiotics, Antitubercular therapeutic use, DNA, Complementary biosynthesis, Drug Therapy, Combination, Female, Gene Expression, Humans, Immunohistochemistry, Leprosy genetics, Leprosy mortality, Male, Methylprednisolone therapeutic use, Middle Aged, Prednisolone therapeutic use, Toll-Like Receptor 2 drug effects, Toll-Like Receptor 2 genetics, Toll-Like Receptor 2 metabolism, Toll-Like Receptor 4 drug effects, Toll-Like Receptor 4 genetics, Toll-Like Receptor 4 metabolism, Young Adult, Glucocorticoids therapeutic use, Leprosy drug therapy, Toll-Like Receptor 2 physiology, Toll-Like Receptor 4 physiology

Abstract

Background: Leprosy is complicated by immunological reactions which can occur before, during and after successful completion of multidrug therapy. Genetic studies have suggested that polymorphisms in toll-like receptors (TLRs) may affect the susceptibility of an individual with leprosy to developing Type 1 reactions., Objectives: To examine the gene and protein expression of TLRs in the cutaneous lesions of leprosy Type 1 reactions at the onset of reaction and during systemic corticosteroid therapy., Methods: Patients who were being treated for leprosy type 1 reactions with corticosteroids as part of a randomized controlled trial of corticosteroid treatment had skin biopsies performed before, during and at the end of treatment. The gene and protein expression of TLR2 and TLR4 were measured., Results: We have demonstrated that the gene hARP-P0 is a suitable control gene for TLR gene expression studies in this population. The gene and protein expression of TLR2 and TLR4 were both reduced significantly during corticosteroid treatment., Conclusions: This is the first study to examine the expression of TLR2 and TLR4 in vivo in individuals experiencing leprosy Type 1 reactions. The data support the possibility of an important role for TLR2 and TLR4 in the pathogenesis of this important complication of leprosy., (© 2012 The Authors. BJD © 2012 British Association of Dermatologists.)

Published

2012

33. A comparison of the change in clinical severity scale score and a retrospective physician assessment of neurological outcome in individuals with leprosy associated nerve function impairment after treatment with corticosteroids.

Author

Walker SL, Nicholls PG, Dhakal S, Hawksworth RA, Macdonald M, Mahat K, Ruchal S, Hamal S, Hagge DA, Neupane KD, and Lockwood DN

Subjects

Adolescent, Adult, Aged, Female, Humans, Leprosy physiopathology, Male, Middle Aged, Muscle, Skeletal physiopathology, Nervous System Diseases etiology, Neurologic Examination, Neuroprotective Agents therapeutic use, Prednisolone therapeutic use, Tibial Nerve physiopathology, Trigeminal Nerve physiopathology, Young Adult, Leprosy complications, Methylprednisolone therapeutic use, Nervous System Diseases drug therapy, Nervous System Diseases physiopathology, Severity of Illness Index

Abstract

Objectives: To determine whether the measured change in score of a validated clinical severity scale reflected physician assessed improvement in individuals who had received corticosteroid therapy for leprosy associated nerve damage., Design: Patients with nerve function impairment who participated in a randomised controlled trial of corticosteroids were classified into two groups using a retrospectively determined physician assessment of improvement. One group consisted of patients who had recovered or improved the other of patients who were unchanged or had deteriorated. The change in the clinical severity scale scores of these two groups was compared., Results: The change in the clinical severity scale scores of the 34 eligible individuals in the two groups were significantly different (P = 0.003). Individuals in the group who recovered or improved had a greater change in severity score than those whose nerve function was unchanged or deteriorated., Conclusion: The scale for measuring the severity of leprosy Type 1 reactions (T1Rs) and/or nerve function impairment reflects the clinical improvement of individuals with leprosy associated nerve damage.

Published

2012

34. Real-time PCR and high-resolution melt analysis for rapid detection of Mycobacterium leprae drug resistance mutations and strain types.

Author

Li W, Matsuoka M, Kai M, Thapa P, Khadge S, Hagge DA, Brennan PJ, and Vissa V

Subjects

Animals, Anti-Bacterial Agents pharmacology, Humans, Mice, Microbial Sensitivity Tests methods, Mycobacterium leprae drug effects, Polymorphism, Single Nucleotide, Sensitivity and Specificity, Transition Temperature, Drug Resistance, Bacterial, Molecular Diagnostic Techniques methods, Mutation, Missense, Mycobacterium leprae genetics, Real-Time Polymerase Chain Reaction methods

Abstract

Drug resistance surveillance and strain typing of Mycobacterium leprae are necessary to investigate ongoing transmission of leprosy in regions of endemicity. To enable wider implementation of these molecular analyses, novel real-time PCR-high-resolution melt (RT-PCR-HRM) assays without allele-specific primers or probes and post-PCR sample handling were developed. For the detection of mutations within drug resistance-determining regions (DRDRs) of folP1, rpoB, and gyrA, targets for dapsone, rifampin, and fluoroquinolones, real-time PCR-HRM assays were developed. Wild-type and drug-resistant mouse footpad-derived strains that included three folP1, two rpoB, and one gyrA mutation types in a reference panel were tested. RT-PCR-HRM correctly distinguished the wild type from the mutant strains. In addition, RT-PCR-HRM analyses aided in recognizing samples with mixed or minor alleles and also a mislabeled sample. When tested in 121 sequence-characterized clinical strains, HRM identified all the folP1 mutants representing two mutation types, including one not within the reference panel. The false positives (<5%) could be attributed to low DNA concentration or PCR inhibition. A second set of RT-PCR-HRM assays for identification of three previously reported single nucleotide polymorphisms (SNPs) that have been used for strain typing were developed and validated in 22 reference and 25 clinical strains. Real-time PCR-HRM is a sensitive, simple, rapid, and high-throughput tool for routine screening known DRDR mutants in new and relapsed cases, SNP typing, and detection of minor mutant alleles in the wild-type background at lower costs than current methods and with the potential for quality control in leprosy investigations.

Published

2012

35. Human beta-defensin 3 is up-regulated in cutaneous leprosy type 1 reactions.

Author

Cogen AL, Walker SL, Roberts CH, Hagge DA, Neupane KD, Khadge S, and Lockwood DN

Subjects

Adrenal Cortex Hormones therapeutic use, Biopsy, Cells, Cultured, Gene Expression Profiling, Humans, Immunosuppressive Agents therapeutic use, Keratinocytes immunology, Keratinocytes microbiology, Macrophages immunology, Macrophages microbiology, Real-Time Polymerase Chain Reaction, Leprosy, Lepromatous immunology, Mycobacterium leprae immunology, Up-Regulation, beta-Defensins biosynthesis

Abstract

Background: Leprosy, a chronic granulomatous disease affecting the skin and nerves, is caused by Mycobacterium leprae (M. leprae). The type of leprosy developed depends upon the host immune response. Type 1 reactions (T1Rs), that complicate borderline and lepromatous leprosy, are due to an increase in cell-mediated immunity and manifest as nerve damage and skin inflammation. Owing to the increase in inflammation in the skin of patients with T1Rs, we sought to investigate the activation of the innate immune system during reactionary events. Specifically, we investigated the expression levels of human beta-defensins (hBDs) 2 and 3 in the skin of patients with T1Rs, in keratinocytes, and in macrophages stimulated with M. leprae and corticosteroids., Results: Skin biopsies from twenty-three patients with Type 1 reactions were found to have higher transcript levels of hBD3 as compared to fifteen leprosy patients without Type 1 reactions, as measured by qPCR. Moreover, we observed that keratinocytes but not macrophages up-regulated hBD2 and hBD3 in response to M. leprae stimulation in vitro. Corticosteroid treatment of patients with T1Rs caused a suppression of hBD2 and hBD3 in skin biopsies, as measured by qPCR. In vitro, corticosteroids suppressed M. leprae-dependent induction of hBD2 and hBD3 in keratinocytes., Conclusions: This study demonstrates that hBD3 is induced in leprosy Type 1 Reactions and suppressed by corticosteroids. Furthermore, our findings demonstrate that keratinocytes are responsive to M. leprae and lend support for additional studies on keratinocyte innate immunity in leprosy and T1Rs., Trial Registration: Controlled-Trials.com ISRCTN31894035.

Published

2012

36. Immunogenicity of Mycobacterium leprae unique antigens in leprosy endemic populations in Asia and Africa.

Author

Bobosha K, Van Der Ploeg-Van Schip JJ, Zewdie M, Sapkota BR, Hagge DA, Franken KL, Inbiale W, Aseffa A, Ottenhoff TH, and Geluk A

Subjects

Adult, Africa epidemiology, Asia epidemiology, Bacterial Proteins genetics, Bacterial Proteins immunology, Endemic Diseases, Female, Humans, Interferon-gamma immunology, Leprosy diagnosis, Leprosy epidemiology, Leprosy microbiology, Male, Middle Aged, Mycobacterium leprae genetics, Mycobacterium leprae isolation & purification, Antigens, Bacterial immunology, Leprosy immunology, Mycobacterium leprae immunology

Abstract

Ongoing transmission of leprosy is evident from the stable disease incidence in high burden areas. Tools for early detection of Mycobacterium leprae (M. leprae) infection, particularly in sub-clinically infected individuals, are urgently required to reduce transmission. Following the sequencing of the M. leprae genome, many M. leprae-unique candidate proteins have been identified, several of which have been tested for induction of M. leprae specific T cell responses in different leprosy endemic areas. In this study, 21 M. leprae-unique proteins and 10 peptide pools covering the complete sequence of five M. leprae-unique proteins (ML0576, ML1989, ML1990, ML2283, and ML2567) were evaluated in 160 individuals in Nepal and Ethiopia. These included: tuberculoid and borderline tuberculoid (TT/BT), borderline borderline and borderline lepromatous (BB/BL) leprosy patients; healthy household contacts (HHC); tuberculosis (TB) patients and endemic controls (EC). Immunogenicity of the proteins was determined by IFN-gamma secretion via stimulation of PBMC in 6 days lymphocyte stimulation tests (LST) or in whole blood assays (WBA). In LST, BB/BL patients (40%) responded to ML0573 and ML1601 whereas ML1604 was most immunogenic in TT/BT (35%) and HHC (36%). Additionally, significant numbers of EC displayed IFN-gamma production in response to ML0573 (54%), ML1601 (50%) and ML1604 (54%). TB patients on the other hand, hardly responded to any of the proteins except for ML1989. Comparison of IFN-gamma responses to ML0121, ML0141 and ML0188 for TT/BT patients showed specific increase in diluted 6 days WBA compared to the undiluted 24 hours WBA, whereas EC showed a reduced response in the diluted WBA, which may indicate detection of disease-specific responses in the 6 days WBA. In summary, identification of multiple M. leprae proteins inducing M. leprae-specific T cell responses in groups at high risk of developing leprosy may contribute to improve early detection for M. leprae infection.

Published

2011

37. A phase two randomised controlled double blind trial of high dose intravenous methylprednisolone and oral prednisolone versus intravenous normal saline and oral prednisolone in individuals with leprosy type 1 reactions and/or nerve function impairment.

Author

Walker SL, Nicholls PG, Dhakal S, Hawksworth RA, Macdonald M, Mahat K, Ruchal S, Hamal S, Hagge DA, Neupane KD, and Lockwood DN

Subjects

Adolescent, Adult, Aged, Double-Blind Method, Humans, Injections, Intravenous, Male, Middle Aged, Treatment Outcome, Young Adult, Immunosuppressive Agents administration & dosage, Leprosy complications, Methylprednisolone administration & dosage, Peripheral Nervous System Diseases drug therapy, Prednisolone administration & dosage

Abstract

Background: Leprosy Type 1 reactions are a major cause of nerve damage and the preventable disability that results. Type 1 reactions are treated with oral corticosteroids and there are few data to support the optimal dose and duration of treatment. Type 1 reactions have a Th1 immune profile: cells in cutaneous and neural lesions expressing interferon-γ and interleukin-12. Methylprednisolone has been used in other Th1 mediated diseases such as rheumatoid arthritis in an attempt to switch off the immune response and so we investigated the efficacy of three days of high dose (1 g) intravenous methylprednisolone at the start of prednisolone therapy in leprosy Type 1 reactions and nerve function impairment., Results: Forty-two individuals were randomised to receive methylprednisolone followed by oral prednisolone (n = 20) or oral prednisolone alone (n = 22). There were no significant differences in the rate of adverse events or clinical improvement at the completion of the study. However individuals treated with methylprednisolone were less likely than those treated with prednisolone alone to experience deterioration in sensory function between day 29 and day 113 of the study. The study also demonstrated that 50% of individuals with Type 1 reactions and/or nerve function impairment required additional prednisolone despite treatment with 16 weeks of corticosteroids., Conclusions: The study lends further support to the use of more prolonged courses of corticosteroid to treat Type 1 reactions and the investigation of risk factors for the recurrence of Type 1 reaction and nerve function impairment during and after a corticosteroid treatment., Trial Registration: Controlled-Trials.com ISRCTN31894035.

Published

2011

38. Common polymorphisms in the NOD2 gene region are associated with leprosy and its reactive states.

Author

Berrington WR, Macdonald M, Khadge S, Sapkota BR, Janer M, Hagge DA, Kaplan G, and Hawn TR

Subjects

Adult, Alleles, Case-Control Studies, Erythema Nodosum genetics, Female, Genetic Association Studies, Genetic Predisposition to Disease genetics, Genotype, Haplotypes genetics, Humans, Leprosy, Lepromatous genetics, Male, Middle Aged, Nepal, Nod2 Signaling Adaptor Protein physiology, Leprosy genetics, Nod2 Signaling Adaptor Protein genetics, Polymorphism, Single Nucleotide genetics

Abstract

Background: Because of its wide spectrum of clinical manifestations and its well-defined immunological complications, leprosy is a useful disease for studying genetic regulation of the host response to infection. We hypothesized that polymorphisms in the nucleotide-binding oligomerization domain containing 2 (NOD2) gene, for a cytosolic receptor known to detect mycobacteria, are associated with susceptibility to leprosy and its clinical outcomes., Methods: We used a case-control study design with 933 patients in Nepal. Our study included 240 patients with type 1 (reversal) reactions and 124 patients with type 2 (erythema nodosum leprosum) reactions. We compared the frequencies of 32 common polymorphisms in the NOD2 gene region between patients with the different clinical types of leprosy as well as between the patients and 101 control participants without leprosy., Results: Four polymorphisms were associated with susceptibility to leprosy when comparing allele frequencies, and 8 were associated when comparing genotype frequencies with a dominant model. Five polymorphisms were associated with protection from reversal reaction in an allelic analysis, and 7 were associated with reversal reaction with a dominant model. Four polymorphisms were associated with increased susceptibility to erythema nodosum leprosum in an allelic analysis, whereas 7 of 32 polymorphisms were associated with a dominant model., Conclusion: These data suggest that NOD2 genetic variants are associated with susceptibility to leprosy and the development of leprosy reactive states.

Published

2010

39. The lta4h locus modulates susceptibility to mycobacterial infection in zebrafish and humans.

Author

Tobin DM, Vary JC Jr, Ray JP, Walsh GS, Dunstan SJ, Bang ND, Hagge DA, Khadge S, King MC, Hawn TR, Moens CB, and Ramakrishnan L

Subjects

Animals, Disease Models, Animal, Fish Diseases immunology, Genetic Predisposition to Disease, Humans, Leprosy immunology, Tuberculosis immunology, Zebrafish, Epoxide Hydrolases genetics, Fish Diseases genetics, Leprosy genetics, Tuberculosis genetics

Abstract

Exposure to Mycobacterium tuberculosis produces varied early outcomes, ranging from resistance to infection to progressive disease. Here we report results from a forward genetic screen in zebrafish larvae that identify multiple mutant classes with distinct patterns of innate susceptibility to Mycobacterium marinum. A hypersusceptible mutant maps to the lta4h locus encoding leukotriene A(4) hydrolase, which catalyzes the final step in the synthesis of leukotriene B(4) (LTB(4)), a potent chemoattractant and proinflammatory eicosanoid. lta4h mutations confer hypersusceptibility independent of LTB(4) reduction, by redirecting eicosanoid substrates to anti-inflammatory lipoxins. The resultant anti-inflammatory state permits increased mycobacterial proliferation by limiting production of tumor necrosis factor. In humans, we find that protection from both tuberculosis and multibacillary leprosy is associated with heterozygosity for LTA4H polymorphisms that have previously been correlated with differential LTB(4) production. Our results suggest conserved roles for balanced eicosanoid production in vertebrate resistance to mycobacterial infection., ((c) 2010 Elsevier Inc. All rights reserved.)

Published

2010

40. Lymphotoxin-alpha and TNF have essential but independent roles in the evolution of the granulomatous response in experimental leprosy.

Author

Hagge DA, Saunders BM, Ebenezer GJ, Ray NA, Marks VT, Britton WJ, Krahenbuhl JL, and Adams LB

Subjects

Animals, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Cytokines biosynthesis, Cytokines immunology, Flow Cytometry, Granuloma, Immunohistochemistry, Leprosy genetics, Leprosy pathology, Lymphocyte Activation immunology, Lymphotoxin-alpha genetics, Mice, Mice, Knockout, Receptors, Tumor Necrosis Factor immunology, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha deficiency, Tumor Necrosis Factor-alpha genetics, Leprosy immunology, Lymphotoxin-alpha immunology, Tumor Necrosis Factor-alpha immunology

Abstract

Recent studies identified an association between genetic variants in the lymphotoxin-alpha (LTalpha) gene and leprosy. To study the influence of LTalpha on the control of experimental leprosy, both low- and high-dose Mycobacterium leprae foot pad (FP) infections were evaluated in LTalpha-deficient chimeric (cLTalpha(-/-)) and control chimeric (cB6) mice. Cellular responses to low-dose infection in cLTalpha(-/-) mice were dramatically different, with reduced accumulation of CD4(+) and CD8(+) lymphocytes and macrophages and failure to form granulomas. Growth of M. leprae was contained for 6 months, but augmented late in infection. In contrast, tumor necrosis factor knockout and tumor necrosis factor receptor 1 knockout FPs exhibited extensive inflammatory infiltration with an increase in M. leprae growth throughout infection. Following high-dose infection, cB6 FP induration peaked at 4 weeks and was maintained for 12 weeks. Induration was not sustained in cLTalpha(-/-) FPs that contained few lymphocytes and no granulomas. There was a reduction in the expression levels of inflammatory cytokines, chemokines, and chemokine receptors, including nitric oxide synthase 2, vascular cell adhesion molecule, and intercellular cell adhesion molecule. Furthermore, cLTalpha(-/-) popliteal lymph nodes contained a higher proportion of naïve CD44(lo)CD62L(hi) T cells than cB6 mice, suggestive of reduced T cell activation. Therefore, both LTalpha and tumor necrosis factor are essential for the regulation of the granuloma, but they have distinctive roles in the recruitment of lymphocytes and maintenance of the granulomatous response during chronic M. leprae infection.

Published

2009

41. Emergence of an effective adaptive cell mediated immune response to Mycobacterium leprae is not impaired in reactive oxygen intermediate-deficient mice.

Author

Hagge DA, Marks VT, Ray NA, Dietrich MA, Kearney MT, Scollard DM, Krahenbuhl JL, and Adams LB

Subjects

Animals, Cytokines biosynthesis, Immunity, Cellular, Macrophages immunology, Mice, Mice, Inbred C57BL, Reactive Nitrogen Species metabolism, Mycobacterium leprae immunology, NADPH Oxidases physiology, Reactive Oxygen Species metabolism

Abstract

Cytokine-activated macrophages (MPhi) employ reactive oxygen intermediates (ROI) and reactive nitrogen intermediates (RNI) to combat pathogens. The requirement for ROI for an effective host response to experimental leprosy using mice which have a disruption in the 91-kD subunit of the NAPDH oxidase cytochrome b (phox91-/-) was examined. Mycobacterium leprae multiplication in phox91-/- foot pads (FP) was elevated early in infection but subsequently arrested similarly to control mice within a noninvasive granuloma. Using a modified lepromin test model, a similar cellular composition in the M. leprae-induced FP granuloma in both strains with lymphocyte infiltration consisting primarily of CD4+CD44(hi)CD62L(lo) effector cells was found. Of great interest was the disparity in the T cell population between the granuloma and the draining lymph node which contained predominantly naïve CD4+CD44(lo)CD62L(hi) cells and was, therefore, not representative of the infection site. TH1 cytokines, chemokines and inducible nitric oxide synthase were comparably expressed in the FP of both strains. When infected in vitro, normal MPhi from B6 and phox91-/- mice supported bacterial viability, whereas IFNgamma-activated MPhi killed M. leprae in a RNI-dependent manner, emphasizing that ROI was dispensable. These data show that phox91-/- mice generate a strong adaptive immune response and control long-term infection with M. leprae.

Published

2007

42. An in vitro model for the lepromatous leprosy granuloma: fate of Mycobacterium leprae from target macrophages after interaction with normal and activated effector macrophages.

Author

Hagge DA, Ray NA, Krahenbuhl JL, and Adams LB

Subjects

Animals, Cells, Cultured, Coculture Techniques, Interferon-gamma pharmacology, Leprosy, Lepromatous immunology, Macrophage Activation, Macrophages immunology, Macrophages metabolism, Mice, Mice, Inbred C57BL, Mice, Nude, Mycobacterium leprae metabolism, Reactive Nitrogen Species metabolism, Tumor Necrosis Factor-alpha pharmacology, Cell Communication immunology, Granuloma etiology, Granuloma immunology, Leprosy, Lepromatous microbiology, Macrophages microbiology, Mycobacterium leprae immunology

Abstract

The lepromatous leprosy granuloma is a dynamic entity requiring a steady influx of macrophages (Mphi) for its maintenance. We have developed an in vitro model to study the fate of Mycobacterium leprae in a LL lesion, with and without immunotherapeutic intervention. Target cells, consisting of granuloma Mphi harvested from the footpads of M. leprae-infected athymic nu/nu mice, were cocultured with normal or IFN-gamma-activated (ACT) effector Mphi. The bacilli were recovered and assessed for viability by radiorespirometry. M. leprae recovered from target Mphi possessed high metabolic activity, indicating a viable state in this uncultivable organism. M. leprae recovered from target Mphi incubated with normal effector Mphi exhibited significantly higher metabolism. In contrast, bacilli recovered from target Mphi cocultured with ACT effector Mphi displayed a markedly decreased metabolic activity. Inhibition by ACT Mphi required an E:T ratio of at least 5:1, a coculture incubation period of 3-5 days, and the production of reactive nitrogen intermediates, but not reactive oxygen intermediates. Neither IFN-gamma nor TNF-alpha were required during the cocultivation period. However, cell-to-cell contact between the target and effector Mphi was necessary for augmentation of M. leprae metabolism by normal effector Mphi as well as for inhibition of M. leprae by ACT effector Mphi. Conventional fluorescence microscopy and confocal fluorescence microscopy revealed that the bacilli from the target Mphi were acquired by the effector Mphi. Thus, the state of Mphi infiltrating the granuloma may markedly affect the viability of M. leprae residing in Mphi in the lepromatous lesion.

Published

2004

43. A new model for studying the effects of Mycobacterium leprae on Schwann cell and neuron interactions.

Author

Hagge DA, Oby Robinson S, Scollard D, McCormick G, and Williams DL

Subjects

Animals, Cells, Cultured, Humans, Leprosy microbiology, Leprosy pathology, Mice, Mice, Nude, Microscopy, Electron, Scanning, Models, Neurological, Mycobacterium leprae growth & development, Neurons pathology, Neurons physiology, Rats, Schwann Cells pathology, Schwann Cells physiology, Schwann Cells ultrastructure, Cell Communication physiology, Mycobacterium leprae physiology, Neurons microbiology, Schwann Cells microbiology

Abstract

Millions of patients with leprosy suffer from nerve damage resulting in disabilities as a consequence of Mycobacterium leprae infection. However, mechanisms of nerve damage have not been elucidated because of the lack of a model that maintains M. leprae viability and mimics disease conditions. A model was developed using viable M. leprae, rat Schwann cells, and Schwann cell-neuron cocultures incubated at 33 degrees C. M. leprae retained 56% viability in Schwann cells for 3 weeks after infection at 33 degrees C, compared with 3.6% viability at 37 degrees C. Infected Schwann cells had altered morphology and expression of genes encoding cellular adhesion molecules at 33 degrees C but were capable of interacting with and myelinating neurons. Cocultures, infected after myelination occurred, showed no morphological changes in myelin architecture after 1 month of incubation at 33 degrees C, and M. leprae retained 53% viability. This article describes a new model for studying the effects of M. leprae on Schwann cells.

Published

2002