Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses

Brandon McLeod; Moustafa T. Mabrouk; Kazutoyo Miura; Rashmi Ravichandran; Sally Kephart; Sophia Hailemariam; Thao P. Pham; Anthony Semesi; Iga Kucharska; Prasun Kundu; Wei Chiao Huang; Max Johnson; Alyssa Blackstone; Deleah Pettie; Michael Murphy; John C. Kraft; Elizabeth M. Leaf; Yang Jiao; Marga van de Vegte-Bolmer; Geert Jan van Gemert; Jordache Ramjith; C. Richter King; Randall S. MacGill; Yimin Wu; Kelly K. Lee; Matthijs M. Jore; Neil P. King; Jonathan F. Lovell; Jean Philippe Julien

doi:10.1016/j.immuni.2022.07.015

Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses

Brandon McLeod
, Moustafa T. Mabrouk
, Kazutoyo Miura
, Rashmi Ravichandran
, Sally Kephart
, Sophia Hailemariam
, Thao P. Pham
, Anthony Semesi
, Iga Kucharska
, Prasun Kundu
, Wei Chiao Huang
, Max Johnson
, Alyssa Blackstone
, Deleah Pettie
, Michael Murphy
, John C. Kraft
, Elizabeth M. Leaf
, Yang Jiao
, Marga van de Vegte-Bolmer
, Geert Jan van Gemert

Jordache Ramjith, C. Richter King, Randall S. MacGill, Yimin Wu, Kelly K. Lee, Matthijs M. Jore, Neil P. King, Jonathan F. Lovell, Jean Philippe Julien

Department of Biomedical Engineering

University of Toronto
SUNY Buffalo
National Institutes of Health
University of Washington
Radboud University Nijmegen
PATH’s Malaria Vaccine Initiative (MVI)

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

42 Scopus citations

Abstract

Malaria transmission-blocking vaccines (TBVs) aim to elicit human antibodies that inhibit sporogonic development of Plasmodium falciparum in mosquitoes, thereby preventing onward transmission. Pfs48/45 is a leading clinical TBV candidate antigen and is recognized by the most potent transmission-blocking monoclonal antibody (mAb) yet described; still, clinical development of Pfs48/45 antigens has been hindered, largely by its poor biochemical characteristics. Here, we used structure-based computational approaches to design Pfs48/45 antigens stabilized in the conformation recognized by the most potently inhibitory mAb, achieving >25°C higher thermostability compared with the wild-type protein. Antibodies elicited in mice immunized with these engineered antigens displayed on liposome-based or protein nanoparticle-based vaccine platforms exhibited 1–2 orders of magnitude superior transmission-reducing activity, compared with immunogens bearing the wild-type antigen, driven by improved antibody quality. Our data provide the founding principles for using molecular stabilization solely from antibody structure-function information to drive improved immune responses against a parasitic vaccine target.

Original language	English
Pages (from-to)	1680-1692.e8
Journal	Immunity
Volume	55
Issue number	9
DOIs	https://doi.org/10.1016/j.immuni.2022.07.015
State	Published - Sep 13 2022

Keywords

antibodies
malaria
structure-based immunogen design

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10.1016/j.immuni.2022.07.015

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McLeod, B., Mabrouk, M. T., Miura, K., Ravichandran, R., Kephart, S., Hailemariam, S., Pham, T. P., Semesi, A., Kucharska, I., Kundu, P., Huang, W. C., Johnson, M., Blackstone, A., Pettie, D., Murphy, M., Kraft, J. C., Leaf, E. M., Jiao, Y., van de Vegte-Bolmer, M., ... Julien, J. P. (2022). Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses. Immunity, 55(9), 1680-1692.e8. https://doi.org/10.1016/j.immuni.2022.07.015

@article{51d832d28c7743f8bc13694d4af10cf6,

title = "Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses",

abstract = "Malaria transmission-blocking vaccines (TBVs) aim to elicit human antibodies that inhibit sporogonic development of Plasmodium falciparum in mosquitoes, thereby preventing onward transmission. Pfs48/45 is a leading clinical TBV candidate antigen and is recognized by the most potent transmission-blocking monoclonal antibody (mAb) yet described; still, clinical development of Pfs48/45 antigens has been hindered, largely by its poor biochemical characteristics. Here, we used structure-based computational approaches to design Pfs48/45 antigens stabilized in the conformation recognized by the most potently inhibitory mAb, achieving >25°C higher thermostability compared with the wild-type protein. Antibodies elicited in mice immunized with these engineered antigens displayed on liposome-based or protein nanoparticle-based vaccine platforms exhibited 1–2 orders of magnitude superior transmission-reducing activity, compared with immunogens bearing the wild-type antigen, driven by improved antibody quality. Our data provide the founding principles for using molecular stabilization solely from antibody structure-function information to drive improved immune responses against a parasitic vaccine target.",

keywords = "antibodies, malaria, structure-based immunogen design",

author = "Brandon McLeod and Mabrouk, \{Moustafa T.\} and Kazutoyo Miura and Rashmi Ravichandran and Sally Kephart and Sophia Hailemariam and Pham, \{Thao P.\} and Anthony Semesi and Iga Kucharska and Prasun Kundu and Huang, \{Wei Chiao\} and Max Johnson and Alyssa Blackstone and Deleah Pettie and Michael Murphy and Kraft, \{John C.\} and Leaf, \{Elizabeth M.\} and Yang Jiao and \{van de Vegte-Bolmer\}, Marga and \{van Gemert\}, \{Geert Jan\} and Jordache Ramjith and King, \{C. Richter\} and MacGill, \{Randall S.\} and Yimin Wu and Lee, \{Kelly K.\} and Jore, \{Matthijs M.\} and King, \{Neil P.\} and Lovell, \{Jonathan F.\} and Julien, \{Jean Philippe\}",

note = "Publisher Copyright: {\textcopyright} 2022 The Author(s)",

year = "2022",

month = sep,

day = "13",

doi = "10.1016/j.immuni.2022.07.015",

language = "English",

volume = "55",

pages = "1680--1692.e8",

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McLeod, B, Mabrouk, MT, Miura, K, Ravichandran, R, Kephart, S, Hailemariam, S, Pham, TP, Semesi, A, Kucharska, I, Kundu, P, Huang, WC, Johnson, M, Blackstone, A, Pettie, D, Murphy, M, Kraft, JC, Leaf, EM, Jiao, Y, van de Vegte-Bolmer, M, van Gemert, GJ, Ramjith, J, King, CR, MacGill, RS, Wu, Y, Lee, KK, Jore, MM, King, NP, Lovell, JF & Julien, JP 2022, 'Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses', Immunity, vol. 55, no. 9, pp. 1680-1692.e8. https://doi.org/10.1016/j.immuni.2022.07.015

TY - JOUR

T1 - Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses

AU - McLeod, Brandon

AU - Mabrouk, Moustafa T.

AU - Miura, Kazutoyo

AU - Ravichandran, Rashmi

AU - Kephart, Sally

AU - Hailemariam, Sophia

AU - Pham, Thao P.

AU - Semesi, Anthony

AU - Kucharska, Iga

AU - Kundu, Prasun

AU - Huang, Wei Chiao

AU - Johnson, Max

AU - Blackstone, Alyssa

AU - Pettie, Deleah

AU - Murphy, Michael

AU - Kraft, John C.

AU - Leaf, Elizabeth M.

AU - Jiao, Yang

AU - van de Vegte-Bolmer, Marga

AU - van Gemert, Geert Jan

AU - Ramjith, Jordache

AU - King, C. Richter

AU - MacGill, Randall S.

AU - Wu, Yimin

AU - Lee, Kelly K.

AU - Jore, Matthijs M.

AU - King, Neil P.

AU - Lovell, Jonathan F.

AU - Julien, Jean Philippe

PY - 2022/9/13

Y1 - 2022/9/13

N2 - Malaria transmission-blocking vaccines (TBVs) aim to elicit human antibodies that inhibit sporogonic development of Plasmodium falciparum in mosquitoes, thereby preventing onward transmission. Pfs48/45 is a leading clinical TBV candidate antigen and is recognized by the most potent transmission-blocking monoclonal antibody (mAb) yet described; still, clinical development of Pfs48/45 antigens has been hindered, largely by its poor biochemical characteristics. Here, we used structure-based computational approaches to design Pfs48/45 antigens stabilized in the conformation recognized by the most potently inhibitory mAb, achieving >25°C higher thermostability compared with the wild-type protein. Antibodies elicited in mice immunized with these engineered antigens displayed on liposome-based or protein nanoparticle-based vaccine platforms exhibited 1–2 orders of magnitude superior transmission-reducing activity, compared with immunogens bearing the wild-type antigen, driven by improved antibody quality. Our data provide the founding principles for using molecular stabilization solely from antibody structure-function information to drive improved immune responses against a parasitic vaccine target.

AB - Malaria transmission-blocking vaccines (TBVs) aim to elicit human antibodies that inhibit sporogonic development of Plasmodium falciparum in mosquitoes, thereby preventing onward transmission. Pfs48/45 is a leading clinical TBV candidate antigen and is recognized by the most potent transmission-blocking monoclonal antibody (mAb) yet described; still, clinical development of Pfs48/45 antigens has been hindered, largely by its poor biochemical characteristics. Here, we used structure-based computational approaches to design Pfs48/45 antigens stabilized in the conformation recognized by the most potently inhibitory mAb, achieving >25°C higher thermostability compared with the wild-type protein. Antibodies elicited in mice immunized with these engineered antigens displayed on liposome-based or protein nanoparticle-based vaccine platforms exhibited 1–2 orders of magnitude superior transmission-reducing activity, compared with immunogens bearing the wild-type antigen, driven by improved antibody quality. Our data provide the founding principles for using molecular stabilization solely from antibody structure-function information to drive improved immune responses against a parasitic vaccine target.

KW - antibodies

KW - malaria

KW - structure-based immunogen design

UR - https://www.scopus.com/pages/publications/85137607354

U2 - 10.1016/j.immuni.2022.07.015

DO - 10.1016/j.immuni.2022.07.015

M3 - Article

C2 - 35977542

AN - SCOPUS:85137607354

SN - 1074-7613

VL - 55

SP - 1680-1692.e8

JO - Immunity

JF - Immunity

IS - 9

ER -

Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses

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Keywords

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