Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation

Ahmet Arac; Sara E. Brownell; Jonathan B. Rothbard; Charlene Chen; Rose M. Ko; Marta P. Pereira; Gregory W. Albers; Lawrence Steinman; Gary K. Steinberg

doi:10.1073/pnas.1107368108

Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation

Ahmet Arac, Sara E. Brownell, Jonathan B. Rothbard, Charlene Chen, Rose M. Ko, Marta P. Pereira, Gregory W. Albers, Lawrence Steinman, Gary K. Steinberg

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

120 Scopus citations

Abstract

Tissue plasminogen activator is the only treatment option for stroke victims; however, it has to be administered within 4.5 h after symptom onset, making its use very limited. This report describes a unique target for effective treatment of stroke, even 12 h after onset, by the administration of αB-crystallin (Cryab), an endogenous immunomodulatory neuroprotectant. In Cryab ^-/- mice, there was increased lesion size and diminished neurologic function after stroke compared with wild-type mice. Increased plasma Cryab was detected after experimental stroke in mice and after stroke in human patients. Administration of Cryab even 12 h after experimental stroke reduced both stroke volume and inflammatory cytokines associated with stroke pathology. Cryab is an endogenous anti-inflammatory and neuroprotectant molecule produced after stroke, whose beneficial properties can be augmented when administered therapeutically after stroke.

Original language	English (US)
Pages (from-to)	13287-13292
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	108
Issue number	32
DOIs	https://doi.org/10.1073/pnas.1107368108
State	Published - Aug 9 2011
Externally published	Yes

Keywords

Immune system
Ischemic stroke

ASJC Scopus subject areas

General

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10.1073/pnas.1107368108

Cite this

Arac, A., Brownell, S. E., Rothbard, J. B., Chen, C., Ko, R. M., Pereira, M. P., Albers, G. W., Steinman, L., & Steinberg, G. K. (2011). Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation. Proceedings of the National Academy of Sciences of the United States of America, 108(32), 13287-13292. https://doi.org/10.1073/pnas.1107368108

Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation. / Arac, Ahmet; Brownell, Sara E.; Rothbard, Jonathan B. et al.
In: Proceedings of the National Academy of Sciences of the United States of America, Vol. 108, No. 32, 09.08.2011, p. 13287-13292.

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

Arac, A, Brownell, SE, Rothbard, JB, Chen, C, Ko, RM, Pereira, MP, Albers, GW, Steinman, L & Steinberg, GK 2011, 'Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation', Proceedings of the National Academy of Sciences of the United States of America, vol. 108, no. 32, pp. 13287-13292. https://doi.org/10.1073/pnas.1107368108

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abstract = "Tissue plasminogen activator is the only treatment option for stroke victims; however, it has to be administered within 4.5 h after symptom onset, making its use very limited. This report describes a unique target for effective treatment of stroke, even 12 h after onset, by the administration of αB-crystallin (Cryab), an endogenous immunomodulatory neuroprotectant. In Cryab -/- mice, there was increased lesion size and diminished neurologic function after stroke compared with wild-type mice. Increased plasma Cryab was detected after experimental stroke in mice and after stroke in human patients. Administration of Cryab even 12 h after experimental stroke reduced both stroke volume and inflammatory cytokines associated with stroke pathology. Cryab is an endogenous anti-inflammatory and neuroprotectant molecule produced after stroke, whose beneficial properties can be augmented when administered therapeutically after stroke.",

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AU - Ko, Rose M.

AU - Pereira, Marta P.

AU - Albers, Gregory W.

AU - Steinman, Lawrence

AU - Steinberg, Gary K.

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AB - Tissue plasminogen activator is the only treatment option for stroke victims; however, it has to be administered within 4.5 h after symptom onset, making its use very limited. This report describes a unique target for effective treatment of stroke, even 12 h after onset, by the administration of αB-crystallin (Cryab), an endogenous immunomodulatory neuroprotectant. In Cryab -/- mice, there was increased lesion size and diminished neurologic function after stroke compared with wild-type mice. Increased plasma Cryab was detected after experimental stroke in mice and after stroke in human patients. Administration of Cryab even 12 h after experimental stroke reduced both stroke volume and inflammatory cytokines associated with stroke pathology. Cryab is an endogenous anti-inflammatory and neuroprotectant molecule produced after stroke, whose beneficial properties can be augmented when administered therapeutically after stroke.

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Systemic augmentation of αB-crystallin provides therapeutic benefit twelve hours post-stroke onset via immune modulation

Abstract

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