Tregs control the development of symptomatic West Nile virus infection in humans and mice

Marion C. Lanteri; Katie M. O'Brien; Whitney E. Purtha; Mark J. Cameron; Jennifer M. Lund; Rachel E. Owen; John W. Heitman; Brian Custer; Dale F. Hirschkorn; Leslie H. Tobler; Nancy Kiely; Harry E. Prince; Lishomwa C. Ndhlovu; Douglas F. Nixon; Hany T. Kamel; David J. Kelvin; Michael P. Busch; Alexander Y. Rudensky; Michael S. Diamond; Philip J. Norris

doi:10.1172/JCI39387

Tregs control the development of symptomatic West Nile virus infection in humans and mice

Marion C. Lanteri, Katie M. O'Brien, Whitney E. Purtha, Mark J. Cameron, Jennifer M. Lund, Rachel E. Owen, John W. Heitman, Brian Custer, Dale F. Hirschkorn, Leslie H. Tobler, Nancy Kiely, Harry E. Prince, Lishomwa C. Ndhlovu, Douglas F. Nixon, Hany T. Kamel, David J. Kelvin, Michael P. Busch, Alexander Y. Rudensky, Michael S. Diamond, Philip J. Norris

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192 Citas (Scopus)

Resumen

West Nile virus (WNV) causes asymptomatic infection in most humans, but for undefined reasons, approximately 20% of immunocompetent individuals develop West Nile fever, a potentially debilitating febrile illness, and approximately 1% develop neuroinvasive disease syndromes. Notably, since its emergence in 1999, WNV has become the leading cause of epidemic viral encephalitis in North America. We hypothesized that CD4+ Tregs might be differentially regulated in subjects with symptomatic compared with those with asymptomatic WNV infection. Here, we show that in 32 blood donors with acute WNV infection, Tregs expanded significantly in the 3 months after index (RNA+) donations in all subjects. Symptomatic donors exhibited lower Treg frequencies from 2 weeks through 1 year after index donation yet did not show differences in systemic T cell or generalized inflammatory responses. In parallel prospective experimental studies, symptomatic WNV-infected mice also developed lower Treg frequencies compared with asymptomatic mice at 2 weeks after infection. Moreover, Treg-deficient mice developed lethal WNV infection at a higher rate than controls. Together, these results suggest that higher levels of peripheral Tregs after infection protect against severe WNV disease in immunocompetent animals and humans.

Idioma original	English
Páginas (desde-hasta)	3266-3277
Número de páginas	12
Publicación	Journal of Clinical Investigation
Volumen	119
N.º	11
DOI	https://doi.org/10.1172/JCI39387
Estado	Published - nov. 2 2009
Publicado de forma externa	Sí

ASJC Scopus Subject Areas

General Medicine

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Lanteri, M. C., O'Brien, K. M., Purtha, W. E., Cameron, M. J., Lund, J. M., Owen, R. E., Heitman, J. W., Custer, B., Hirschkorn, D. F., Tobler, L. H., Kiely, N., Prince, H. E., Ndhlovu, L. C., Nixon, D. F., Kamel, H. T., Kelvin, D. J., Busch, M. P., Rudensky, A. Y., Diamond, M. S., & Norris, P. J. (2009). Tregs control the development of symptomatic West Nile virus infection in humans and mice. Journal of Clinical Investigation, 119(11), 3266-3277. https://doi.org/10.1172/JCI39387

Lanteri, MC, O'Brien, KM, Purtha, WE, Cameron, MJ, Lund, JM, Owen, RE, Heitman, JW, Custer, B, Hirschkorn, DF, Tobler, LH, Kiely, N, Prince, HE, Ndhlovu, LC, Nixon, DF, Kamel, HT, Kelvin, DJ, Busch, MP, Rudensky, AY, Diamond, MS & Norris, PJ 2009, 'Tregs control the development of symptomatic West Nile virus infection in humans and mice', Journal of Clinical Investigation, vol. 119, n.º 11, pp. 3266-3277. https://doi.org/10.1172/JCI39387

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abstract = "West Nile virus (WNV) causes asymptomatic infection in most humans, but for undefined reasons, approximately 20% of immunocompetent individuals develop West Nile fever, a potentially debilitating febrile illness, and approximately 1% develop neuroinvasive disease syndromes. Notably, since its emergence in 1999, WNV has become the leading cause of epidemic viral encephalitis in North America. We hypothesized that CD4+ Tregs might be differentially regulated in subjects with symptomatic compared with those with asymptomatic WNV infection. Here, we show that in 32 blood donors with acute WNV infection, Tregs expanded significantly in the 3 months after index (RNA+) donations in all subjects. Symptomatic donors exhibited lower Treg frequencies from 2 weeks through 1 year after index donation yet did not show differences in systemic T cell or generalized inflammatory responses. In parallel prospective experimental studies, symptomatic WNV-infected mice also developed lower Treg frequencies compared with asymptomatic mice at 2 weeks after infection. Moreover, Treg-deficient mice developed lethal WNV infection at a higher rate than controls. Together, these results suggest that higher levels of peripheral Tregs after infection protect against severe WNV disease in immunocompetent animals and humans.",

author = "Lanteri, {Marion C.} and O'Brien, {Katie M.} and Purtha, {Whitney E.} and Cameron, {Mark J.} and Lund, {Jennifer M.} and Owen, {Rachel E.} and Heitman, {John W.} and Brian Custer and Hirschkorn, {Dale F.} and Tobler, {Leslie H.} and Nancy Kiely and Prince, {Harry E.} and Ndhlovu, {Lishomwa C.} and Nixon, {Douglas F.} and Kamel, {Hany T.} and Kelvin, {David J.} and Busch, {Michael P.} and Rudensky, {Alexander Y.} and Diamond, {Michael S.} and Norris, {Philip J.}",

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AU - Lund, Jennifer M.

AU - Owen, Rachel E.

AU - Heitman, John W.

AU - Custer, Brian

AU - Hirschkorn, Dale F.

AU - Tobler, Leslie H.

AU - Kiely, Nancy

AU - Prince, Harry E.

AU - Ndhlovu, Lishomwa C.

AU - Nixon, Douglas F.

AU - Kamel, Hany T.

AU - Kelvin, David J.

AU - Busch, Michael P.

AU - Rudensky, Alexander Y.

AU - Diamond, Michael S.

AU - Norris, Philip J.

PY - 2009/11/2

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N2 - West Nile virus (WNV) causes asymptomatic infection in most humans, but for undefined reasons, approximately 20% of immunocompetent individuals develop West Nile fever, a potentially debilitating febrile illness, and approximately 1% develop neuroinvasive disease syndromes. Notably, since its emergence in 1999, WNV has become the leading cause of epidemic viral encephalitis in North America. We hypothesized that CD4+ Tregs might be differentially regulated in subjects with symptomatic compared with those with asymptomatic WNV infection. Here, we show that in 32 blood donors with acute WNV infection, Tregs expanded significantly in the 3 months after index (RNA+) donations in all subjects. Symptomatic donors exhibited lower Treg frequencies from 2 weeks through 1 year after index donation yet did not show differences in systemic T cell or generalized inflammatory responses. In parallel prospective experimental studies, symptomatic WNV-infected mice also developed lower Treg frequencies compared with asymptomatic mice at 2 weeks after infection. Moreover, Treg-deficient mice developed lethal WNV infection at a higher rate than controls. Together, these results suggest that higher levels of peripheral Tregs after infection protect against severe WNV disease in immunocompetent animals and humans.

AB - West Nile virus (WNV) causes asymptomatic infection in most humans, but for undefined reasons, approximately 20% of immunocompetent individuals develop West Nile fever, a potentially debilitating febrile illness, and approximately 1% develop neuroinvasive disease syndromes. Notably, since its emergence in 1999, WNV has become the leading cause of epidemic viral encephalitis in North America. We hypothesized that CD4+ Tregs might be differentially regulated in subjects with symptomatic compared with those with asymptomatic WNV infection. Here, we show that in 32 blood donors with acute WNV infection, Tregs expanded significantly in the 3 months after index (RNA+) donations in all subjects. Symptomatic donors exhibited lower Treg frequencies from 2 weeks through 1 year after index donation yet did not show differences in systemic T cell or generalized inflammatory responses. In parallel prospective experimental studies, symptomatic WNV-infected mice also developed lower Treg frequencies compared with asymptomatic mice at 2 weeks after infection. Moreover, Treg-deficient mice developed lethal WNV infection at a higher rate than controls. Together, these results suggest that higher levels of peripheral Tregs after infection protect against severe WNV disease in immunocompetent animals and humans.

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Tregs control the development of symptomatic West Nile virus infection in humans and mice

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