Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues

Julia R. Port; David M. Wozniak; Lisa Oestereich; Elisa Pallasch; Beate Becker-Ziaja; Jonas Müller; Monika Rottstegge; Catherine Olal; Sergio Gómez-Medina; Jennifer Oyakhliome; Yemisi Ighodalo; Emmanuel Omomoh; Thomas Olokor; Donatus I. Adomeh; Danny Asogun; Ephraim Ogbani-Emovon; Kristin Hartmann; Susanne Krasemann; Emily V. Nelson; Beatriz Escudero-Pérez; Anita K. McElroy; Stephan Günther; César Muñoz-Fontela

doi:10.1128/JVI.01367-20

Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues

Julia R. Port
, David M. Wozniak
, Lisa Oestereich
, Elisa Pallasch
, Beate Becker-Ziaja
, Jonas Müller
, Monika Rottstegge
, Catherine Olal
, Sergio Gómez-Medina
, Jennifer Oyakhliome
, Yemisi Ighodalo
, Emmanuel Omomoh
, Thomas Olokor
, Donatus I. Adomeh
, Danny Asogun
, Ephraim Ogbani-Emovon
, Kristin Hartmann
, Susanne Krasemann
, Emily V. Nelson
, Beatriz Escudero-Pérez

Anita K. McElroy, Stephan Günther, César Muñoz-Fontela

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

26 Scopus citations

Abstract

Lassa fever (LF) is a zoonotic viral hemorrhagic fever caused by Lassa virus (LASV), which is endemic to West African countries. Previous studies have suggested an important role for T-cell-mediated immunopathology in LF pathogenesis, but the mechanisms by which T cells influence disease severity and outcome are not well understood. Here, we present a multiparametric analysis of clinical immunology data collected during the 2017–2018 Lassa fever outbreak in Nigeria. During the acute phase of LF, we observed robust activation of the polyclonal T-cell repertoire, which included LASV-specific and antigenically unrelated T cells. However, severe and fatal LF cases were characterized by poor LASV-specific effector T-cell responses. Severe LF was also characterized by the presence of circulating T cells with homing capacity to inflamed tissues, including the gut mucosa. These findings in LF patients were recapitulated in a mouse model of LASV infection, in which mucosal exposure resulted in remarkably high lethality compared to skin exposure. Taken together, our findings indicate that poor LASV-specific T-cell responses and activation of nonspecific T cells with homing capacity to inflamed tissues are associated with severe LF. IMPORTANCE Lassa fever may cause severe disease in humans, in particular in areas of endemicity like Sierra Leone and Nigeria. Despite its public health importance, the pathophysiology of Lassa fever in humans is poorly understood. Here, we present clinical immunology data obtained in the field during the 2018 Lassa fever outbreak in Nigeria indicating that severe Lassa fever is associated with activation of T cells antigenically unrelated to Lassa virus and poor Lassa virus-specific effector T-cell responses. Mechanistically, we show that these bystander T cells express defined tissue homing signatures that suggest their recruitment to inflamed tissues and a putative role of these T cells in immunopathology. These findings open a window of opportunity to consider T-cell targeting as a potential postexposure therapeutic strategy against severe Lassa fever, a hypothesis that could be tested in relevant animal models, such as nonhuman primates.

Original language	English
Article number	e01367-20
Journal	Journal of Virology
Volume	94
Issue number	21
DOIs	https://doi.org/10.1128/JVI.01367-20
State	Published - 14 Oct 2020
Externally published	Yes

Keywords

Host response
Lassa fever
Lassa virus
Pathogenesis
T cells
T-cell homing
Viral hemorrhagic fever

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10.1128/JVI.01367-20

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Port, J. R., Wozniak, D. M., Oestereich, L., Pallasch, E., Becker-Ziaja, B., Müller, J., Rottstegge, M., Olal, C., Gómez-Medina, S., Oyakhliome, J., Ighodalo, Y., Omomoh, E., Olokor, T., Adomeh, D. I., Asogun, D., Ogbani-Emovon, E., Hartmann, K., Krasemann, S., Nelson, E. V., ... Muñoz-Fontela, C. (2020). Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues. Journal of Virology, 94(21), Article e01367-20. https://doi.org/10.1128/JVI.01367-20

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title = "Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues",

abstract = "Lassa fever (LF) is a zoonotic viral hemorrhagic fever caused by Lassa virus (LASV), which is endemic to West African countries. Previous studies have suggested an important role for T-cell-mediated immunopathology in LF pathogenesis, but the mechanisms by which T cells influence disease severity and outcome are not well understood. Here, we present a multiparametric analysis of clinical immunology data collected during the 2017–2018 Lassa fever outbreak in Nigeria. During the acute phase of LF, we observed robust activation of the polyclonal T-cell repertoire, which included LASV-specific and antigenically unrelated T cells. However, severe and fatal LF cases were characterized by poor LASV-specific effector T-cell responses. Severe LF was also characterized by the presence of circulating T cells with homing capacity to inflamed tissues, including the gut mucosa. These findings in LF patients were recapitulated in a mouse model of LASV infection, in which mucosal exposure resulted in remarkably high lethality compared to skin exposure. Taken together, our findings indicate that poor LASV-specific T-cell responses and activation of nonspecific T cells with homing capacity to inflamed tissues are associated with severe LF. IMPORTANCE Lassa fever may cause severe disease in humans, in particular in areas of endemicity like Sierra Leone and Nigeria. Despite its public health importance, the pathophysiology of Lassa fever in humans is poorly understood. Here, we present clinical immunology data obtained in the field during the 2018 Lassa fever outbreak in Nigeria indicating that severe Lassa fever is associated with activation of T cells antigenically unrelated to Lassa virus and poor Lassa virus-specific effector T-cell responses. Mechanistically, we show that these bystander T cells express defined tissue homing signatures that suggest their recruitment to inflamed tissues and a putative role of these T cells in immunopathology. These findings open a window of opportunity to consider T-cell targeting as a potential postexposure therapeutic strategy against severe Lassa fever, a hypothesis that could be tested in relevant animal models, such as nonhuman primates.",

keywords = "Host response, Lassa fever, Lassa virus, Pathogenesis, T cells, T-cell homing, Viral hemorrhagic fever",

author = "Port, \{Julia R.\} and Wozniak, \{David M.\} and Lisa Oestereich and Elisa Pallasch and Beate Becker-Ziaja and Jonas M{\"u}ller and Monika Rottstegge and Catherine Olal and Sergio G{\'o}mez-Medina and Jennifer Oyakhliome and Yemisi Ighodalo and Emmanuel Omomoh and Thomas Olokor and Adomeh, \{Donatus I.\} and Danny Asogun and Ephraim Ogbani-Emovon and Kristin Hartmann and Susanne Krasemann and Nelson, \{Emily V.\} and Beatriz Escudero-P{\'e}rez and McElroy, \{Anita K.\} and Stephan G{\"u}nther and C{\'e}sar Mu{\~n}oz-Fontela",

note = "Publisher Copyright: Copyright {\textcopyright} 2020 Port et al.",

year = "2020",

month = oct,

day = "14",

doi = "10.1128/JVI.01367-20",

language = "English",

volume = "94",

journal = "Journal of Virology",

issn = "0022-538X",

publisher = "American Society for Microbiology",

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Port, JR, Wozniak, DM, Oestereich, L, Pallasch, E, Becker-Ziaja, B, Müller, J, Rottstegge, M, Olal, C, Gómez-Medina, S, Oyakhliome, J, Ighodalo, Y, Omomoh, E, Olokor, T, Adomeh, DI, Asogun, D, Ogbani-Emovon, E, Hartmann, K, Krasemann, S, Nelson, EV, Escudero-Pérez, B, McElroy, AK, Günther, S & Muñoz-Fontela, C 2020, 'Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues', Journal of Virology, vol. 94, no. 21, e01367-20. https://doi.org/10.1128/JVI.01367-20

TY - JOUR

T1 - Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues

AU - Port, Julia R.

AU - Wozniak, David M.

AU - Oestereich, Lisa

AU - Pallasch, Elisa

AU - Becker-Ziaja, Beate

AU - Müller, Jonas

AU - Rottstegge, Monika

AU - Olal, Catherine

AU - Gómez-Medina, Sergio

AU - Oyakhliome, Jennifer

AU - Ighodalo, Yemisi

AU - Omomoh, Emmanuel

AU - Olokor, Thomas

AU - Adomeh, Donatus I.

AU - Asogun, Danny

AU - Ogbani-Emovon, Ephraim

AU - Hartmann, Kristin

AU - Krasemann, Susanne

AU - Nelson, Emily V.

AU - Escudero-Pérez, Beatriz

AU - McElroy, Anita K.

AU - Günther, Stephan

AU - Muñoz-Fontela, César

PY - 2020/10/14

Y1 - 2020/10/14

N2 - Lassa fever (LF) is a zoonotic viral hemorrhagic fever caused by Lassa virus (LASV), which is endemic to West African countries. Previous studies have suggested an important role for T-cell-mediated immunopathology in LF pathogenesis, but the mechanisms by which T cells influence disease severity and outcome are not well understood. Here, we present a multiparametric analysis of clinical immunology data collected during the 2017–2018 Lassa fever outbreak in Nigeria. During the acute phase of LF, we observed robust activation of the polyclonal T-cell repertoire, which included LASV-specific and antigenically unrelated T cells. However, severe and fatal LF cases were characterized by poor LASV-specific effector T-cell responses. Severe LF was also characterized by the presence of circulating T cells with homing capacity to inflamed tissues, including the gut mucosa. These findings in LF patients were recapitulated in a mouse model of LASV infection, in which mucosal exposure resulted in remarkably high lethality compared to skin exposure. Taken together, our findings indicate that poor LASV-specific T-cell responses and activation of nonspecific T cells with homing capacity to inflamed tissues are associated with severe LF. IMPORTANCE Lassa fever may cause severe disease in humans, in particular in areas of endemicity like Sierra Leone and Nigeria. Despite its public health importance, the pathophysiology of Lassa fever in humans is poorly understood. Here, we present clinical immunology data obtained in the field during the 2018 Lassa fever outbreak in Nigeria indicating that severe Lassa fever is associated with activation of T cells antigenically unrelated to Lassa virus and poor Lassa virus-specific effector T-cell responses. Mechanistically, we show that these bystander T cells express defined tissue homing signatures that suggest their recruitment to inflamed tissues and a putative role of these T cells in immunopathology. These findings open a window of opportunity to consider T-cell targeting as a potential postexposure therapeutic strategy against severe Lassa fever, a hypothesis that could be tested in relevant animal models, such as nonhuman primates.

AB - Lassa fever (LF) is a zoonotic viral hemorrhagic fever caused by Lassa virus (LASV), which is endemic to West African countries. Previous studies have suggested an important role for T-cell-mediated immunopathology in LF pathogenesis, but the mechanisms by which T cells influence disease severity and outcome are not well understood. Here, we present a multiparametric analysis of clinical immunology data collected during the 2017–2018 Lassa fever outbreak in Nigeria. During the acute phase of LF, we observed robust activation of the polyclonal T-cell repertoire, which included LASV-specific and antigenically unrelated T cells. However, severe and fatal LF cases were characterized by poor LASV-specific effector T-cell responses. Severe LF was also characterized by the presence of circulating T cells with homing capacity to inflamed tissues, including the gut mucosa. These findings in LF patients were recapitulated in a mouse model of LASV infection, in which mucosal exposure resulted in remarkably high lethality compared to skin exposure. Taken together, our findings indicate that poor LASV-specific T-cell responses and activation of nonspecific T cells with homing capacity to inflamed tissues are associated with severe LF. IMPORTANCE Lassa fever may cause severe disease in humans, in particular in areas of endemicity like Sierra Leone and Nigeria. Despite its public health importance, the pathophysiology of Lassa fever in humans is poorly understood. Here, we present clinical immunology data obtained in the field during the 2018 Lassa fever outbreak in Nigeria indicating that severe Lassa fever is associated with activation of T cells antigenically unrelated to Lassa virus and poor Lassa virus-specific effector T-cell responses. Mechanistically, we show that these bystander T cells express defined tissue homing signatures that suggest their recruitment to inflamed tissues and a putative role of these T cells in immunopathology. These findings open a window of opportunity to consider T-cell targeting as a potential postexposure therapeutic strategy against severe Lassa fever, a hypothesis that could be tested in relevant animal models, such as nonhuman primates.

KW - Host response

KW - Lassa fever

KW - Lassa virus

KW - Pathogenesis

KW - T cells

KW - T-cell homing

KW - Viral hemorrhagic fever

UR - https://www.scopus.com/pages/publications/85093538306

U2 - 10.1128/JVI.01367-20

DO - 10.1128/JVI.01367-20

M3 - Article

C2 - 32817220

AN - SCOPUS:85093538306

SN - 0022-538X

VL - 94

JO - Journal of Virology

JF - Journal of Virology

IS - 21

M1 - e01367-20

ER -

Severe Human Lassa Fever Is Characterized by Nonspecific T-Cell Activation and Lymphocyte Homing to Inflamed Tissues

Abstract

Keywords

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