Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes

Ruben Magni; Fatlum Rruga; Fahad Alsaab; Sara Sharif; Marissa Howard; Virginia Espina; Brianna Kim; Benjamin Lepene; Gwenyth Lee; Mohamad A. Alayouni; Hannah Steinberg; Robyn Araujo; Fatah Kashanchi; Fabio Riccardi; Sargento Morreira; Antonia Araujo; Fernando Poli; Devan Jaganath; Fred C. Semitala; William Worodria; Alfred Andama; Alok Choudhary; William J. Honnen; Emanuel F. Petricoin; Adithya Cattamanchi; Raffaella Colombatti; Jacobus H. de Waard; Richard Oberhelman; Abraham Pinter; Robert H. Gilman; Lance A. Liotta; Alessandra Luchini

doi:10.1038/s41598-020-70669-9

Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes

Ruben Magni, Fatlum Rruga, Fahad Alsaab, Sara Sharif, Marissa Howard, Virginia Espina, Brianna Kim, Benjamin Lepene, Gwenyth Lee, Mohamad A. Alayouni, Hannah Steinberg, Robyn Araujo, Fatah Kashanchi, Fabio Riccardi, Sargento Morreira, Antonia Araujo, Fernando Poli, Devan Jaganath, Fred C. Semitala, William WorodriaAlfred Andama, Alok Choudhary, William J. Honnen, Emanuel F. Petricoin, Adithya Cattamanchi, Raffaella Colombatti, Jacobus H. de Waard, Richard Oberhelman, Abraham Pinter, Robert H. Gilman, Lance A. Liotta, Alessandra Luchini

Bloomberg School of Public Health

Research output: Contribution to journal › Article › peer-review

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Abstract

An accurate urine test for diverse populations with active tuberculosis could be transformative for preventing TB deaths. Urinary liporabinomannan (LAM) testing has been previously restricted to HIV co-infected TB patients. In this study we evaluate urinary LAM in HIV negative, pediatric and adult, pulmonary and extrapulmonary tuberculosis patients. We measured 430 microbiologically confirmed pretreatment tuberculosis patients and controls from Peru, Guinea Bissau, Venezuela, Uganda and the United States using three monoclonal antibodies, MoAb1, CS35, and A194, which recognize distinct LAM epitopes, a one-sided immunoassay, and blinded cohorts. We evaluated sources of assay variability and comorbidities (HIV and diabetes). All antibodies successfully discriminated TB positive from TB negative patients. ROAUC from the average of three antibodies’ responses was 0.90; 95% CI 0.87–0.93, 90% sensitivity, 73.5% specificity (80 pg/mL). MoAb1, recognizing the 5-methylthio-d-xylofuranose(MTX)-mannose(Man) cap epitope, performed the best, was less influenced by glycosuria and identified culture positive pediatric (N = 19) and extrapulmonary (N = 24) patients with high accuracy (ROAUC 0.87, 95% CI 0.77–0.98, 0.90 sensitivity 0.80 specificity at 80 pg/mL; ROAUC = 0.96, 95% CI 0.92–0.99, 96% sensitivity, 80% specificity at 82 pg/mL, respectively). The MoAb1 antibody, recognizing the MTX-Man cap epitope, is a novel analyte for active TB detection in pediatric and extrapulmonary disease.

Original language	English (US)
Article number	13944
Journal	Scientific reports
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41598-020-70669-9
State	Published - Dec 1 2020

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Magni, R., Rruga, F., Alsaab, F., Sharif, S., Howard, M., Espina, V., Kim, B., Lepene, B., Lee, G., Alayouni, M. A., Steinberg, H., Araujo, R., Kashanchi, F., Riccardi, F., Morreira, S., Araujo, A., Poli, F., Jaganath, D., Semitala, F. C., ... Luchini, A. (2020). Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes. Scientific reports, 10(1), Article 13944. https://doi.org/10.1038/s41598-020-70669-9

Magni, R, Rruga, F, Alsaab, F, Sharif, S, Howard, M, Espina, V, Kim, B, Lepene, B, Lee, G, Alayouni, MA, Steinberg, H, Araujo, R, Kashanchi, F, Riccardi, F, Morreira, S, Araujo, A, Poli, F, Jaganath, D, Semitala, FC, Worodria, W, Andama, A, Choudhary, A, Honnen, WJ, Petricoin, EF, Cattamanchi, A, Colombatti, R, de Waard, JH, Oberhelman, R, Pinter, A, Gilman, RH, Liotta, LA & Luchini, A 2020, 'Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes', Scientific reports, vol. 10, no. 1, 13944. https://doi.org/10.1038/s41598-020-70669-9

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title = "Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes",

abstract = "An accurate urine test for diverse populations with active tuberculosis could be transformative for preventing TB deaths. Urinary liporabinomannan (LAM) testing has been previously restricted to HIV co-infected TB patients. In this study we evaluate urinary LAM in HIV negative, pediatric and adult, pulmonary and extrapulmonary tuberculosis patients. We measured 430 microbiologically confirmed pretreatment tuberculosis patients and controls from Peru, Guinea Bissau, Venezuela, Uganda and the United States using three monoclonal antibodies, MoAb1, CS35, and A194, which recognize distinct LAM epitopes, a one-sided immunoassay, and blinded cohorts. We evaluated sources of assay variability and comorbidities (HIV and diabetes). All antibodies successfully discriminated TB positive from TB negative patients. ROAUC from the average of three antibodies{\textquoteright} responses was 0.90; 95% CI 0.87–0.93, 90% sensitivity, 73.5% specificity (80 pg/mL). MoAb1, recognizing the 5-methylthio-d-xylofuranose(MTX)-mannose(Man) cap epitope, performed the best, was less influenced by glycosuria and identified culture positive pediatric (N = 19) and extrapulmonary (N = 24) patients with high accuracy (ROAUC 0.87, 95% CI 0.77–0.98, 0.90 sensitivity 0.80 specificity at 80 pg/mL; ROAUC = 0.96, 95% CI 0.92–0.99, 96% sensitivity, 80% specificity at 82 pg/mL, respectively). The MoAb1 antibody, recognizing the MTX-Man cap epitope, is a novel analyte for active TB detection in pediatric and extrapulmonary disease.",

author = "Ruben Magni and Fatlum Rruga and Fahad Alsaab and Sara Sharif and Marissa Howard and Virginia Espina and Brianna Kim and Benjamin Lepene and Gwenyth Lee and Alayouni, {Mohamad A.} and Hannah Steinberg and Robyn Araujo and Fatah Kashanchi and Fabio Riccardi and Sargento Morreira and Antonia Araujo and Fernando Poli and Devan Jaganath and Semitala, {Fred C.} and William Worodria and Alfred Andama and Alok Choudhary and Honnen, {William J.} and Petricoin, {Emanuel F.} and Adithya Cattamanchi and Raffaella Colombatti and {de Waard}, {Jacobus H.} and Richard Oberhelman and Abraham Pinter and Gilman, {Robert H.} and Liotta, {Lance A.} and Alessandra Luchini",

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doi = "10.1038/s41598-020-70669-9",

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AU - Magni, Ruben

AU - Rruga, Fatlum

AU - Alsaab, Fahad

AU - Sharif, Sara

AU - Howard, Marissa

AU - Espina, Virginia

AU - Kim, Brianna

AU - Lepene, Benjamin

AU - Lee, Gwenyth

AU - Alayouni, Mohamad A.

AU - Steinberg, Hannah

AU - Araujo, Robyn

AU - Kashanchi, Fatah

AU - Riccardi, Fabio

AU - Morreira, Sargento

AU - Araujo, Antonia

AU - Poli, Fernando

AU - Jaganath, Devan

AU - Semitala, Fred C.

AU - Worodria, William

AU - Andama, Alfred

AU - Choudhary, Alok

AU - Honnen, William J.

AU - Petricoin, Emanuel F.

AU - Cattamanchi, Adithya

AU - Colombatti, Raffaella

AU - de Waard, Jacobus H.

AU - Oberhelman, Richard

AU - Pinter, Abraham

AU - Gilman, Robert H.

AU - Liotta, Lance A.

AU - Luchini, Alessandra

PY - 2020/12/1

Y1 - 2020/12/1

N2 - An accurate urine test for diverse populations with active tuberculosis could be transformative for preventing TB deaths. Urinary liporabinomannan (LAM) testing has been previously restricted to HIV co-infected TB patients. In this study we evaluate urinary LAM in HIV negative, pediatric and adult, pulmonary and extrapulmonary tuberculosis patients. We measured 430 microbiologically confirmed pretreatment tuberculosis patients and controls from Peru, Guinea Bissau, Venezuela, Uganda and the United States using three monoclonal antibodies, MoAb1, CS35, and A194, which recognize distinct LAM epitopes, a one-sided immunoassay, and blinded cohorts. We evaluated sources of assay variability and comorbidities (HIV and diabetes). All antibodies successfully discriminated TB positive from TB negative patients. ROAUC from the average of three antibodies’ responses was 0.90; 95% CI 0.87–0.93, 90% sensitivity, 73.5% specificity (80 pg/mL). MoAb1, recognizing the 5-methylthio-d-xylofuranose(MTX)-mannose(Man) cap epitope, performed the best, was less influenced by glycosuria and identified culture positive pediatric (N = 19) and extrapulmonary (N = 24) patients with high accuracy (ROAUC 0.87, 95% CI 0.77–0.98, 0.90 sensitivity 0.80 specificity at 80 pg/mL; ROAUC = 0.96, 95% CI 0.92–0.99, 96% sensitivity, 80% specificity at 82 pg/mL, respectively). The MoAb1 antibody, recognizing the MTX-Man cap epitope, is a novel analyte for active TB detection in pediatric and extrapulmonary disease.

AB - An accurate urine test for diverse populations with active tuberculosis could be transformative for preventing TB deaths. Urinary liporabinomannan (LAM) testing has been previously restricted to HIV co-infected TB patients. In this study we evaluate urinary LAM in HIV negative, pediatric and adult, pulmonary and extrapulmonary tuberculosis patients. We measured 430 microbiologically confirmed pretreatment tuberculosis patients and controls from Peru, Guinea Bissau, Venezuela, Uganda and the United States using three monoclonal antibodies, MoAb1, CS35, and A194, which recognize distinct LAM epitopes, a one-sided immunoassay, and blinded cohorts. We evaluated sources of assay variability and comorbidities (HIV and diabetes). All antibodies successfully discriminated TB positive from TB negative patients. ROAUC from the average of three antibodies’ responses was 0.90; 95% CI 0.87–0.93, 90% sensitivity, 73.5% specificity (80 pg/mL). MoAb1, recognizing the 5-methylthio-d-xylofuranose(MTX)-mannose(Man) cap epitope, performed the best, was less influenced by glycosuria and identified culture positive pediatric (N = 19) and extrapulmonary (N = 24) patients with high accuracy (ROAUC 0.87, 95% CI 0.77–0.98, 0.90 sensitivity 0.80 specificity at 80 pg/mL; ROAUC = 0.96, 95% CI 0.92–0.99, 96% sensitivity, 80% specificity at 82 pg/mL, respectively). The MoAb1 antibody, recognizing the MTX-Man cap epitope, is a novel analyte for active TB detection in pediatric and extrapulmonary disease.

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Lipoarabinomannan antigenic epitope differences in tuberculosis disease subtypes

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