Structure-Guided Design of an Anti-dengue Antibody Directed to a Non-immunodominant Epitope | Zendy

Luke N. Robinson | Zendy; Kannan Tharakaraman | Zendy; Kirk J. Rowley | Zendy; Vivian Vasconcelos Costa | Zendy; Kuan Rong Chan | Zendy; Yee Hwa Wong | Zendy; Li Ching Ong | Zendy; Hwee Cheng Tan | Zendy; Tyree Koch | Zendy; David Cain | Zendy; Rama Sanjay Kirloskar | Zendy; Karthik Viswanathan | Zendy; Chong Wai Liew | Zendy; Hamid Tissire | Zendy; Boopathy Ramakrishnan | Zendy; James R. Myette | Zendy; Gregory J. Babcock | Zendy; V. Sasisekharan | Zendy; Sylvie Alonso | Zendy; Jianzhu Chen | Zendy; Julien Lescar | Zendy; Zachary Shriver | Zendy; Eng Eong Ooi | Zendy; Ram Sasisekharan | Zendy

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Structure-Guided Design of an Anti-dengue Antibody Directed to a Non-immunodominant Epitope

Author(s) -

Luke N. Robinson,

Kannan Tharakaraman,

Kirk J. Rowley,

Vivian Vasconcelos Costa,

Kuan Rong Chan,

Yee Hwa Wong,

Li Ching Ong,

Hwee Cheng Tan,

Tyree Koch,

David Cain,

Rama Sanjay Kirloskar,

Karthik Viswanathan,

Chong Wai Liew,

Hamid Tissire,

Boopathy Ramakrishnan,

James R. Myette,

Gregory J. Babcock,

V. Sasisekharan,

Sylvie Alonso,

Jianzhu Chen,

Julien Lescar,

Zachary Shriver,

Eng Eong Ooi,

Ram Sasisekharan

Publication year - 2015

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2015.06.057

Subject(s) - biology , epitope , virology , dengue fever , antibody , dengue vaccine , computational biology , dengue virus , genetics

Dengue is the most common vector-borne viral disease, causing nearly 400 million infections yearly. Currently there are no approved therapies. Antibody epitopes that elicit weak humoral responses may not be accessible by conventional B cell panning methods. To demonstrate an alternative strategy to generating a therapeutic antibody, we employed a non-immunodominant, but functionally relevant, epitope in domain III of the E protein, and engineered by structure-guided methods an antibody directed to it. The resulting antibody, Ab513, exhibits high-affinity binding to, and broadly neutralizes, multiple genotypes within all four serotypes. To assess therapeutic relevance of Ab513, activity against important human clinical features of dengue was investigated. Ab513 mitigates thrombocytopenia in a humanized mouse model, resolves vascular leakage, reduces viremia to nearly undetectable levels, and protects mice in a maternal transfer model of lethal antibody-mediated enhancement. The results demonstrate that Ab513 may reduce the public health burden from dengue.

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