Computational optimization of antibody humanness and stability by systematic energy-based ranking

Ariel Tennenhouse; Lev Khmelnitsky; Razi Khalaila; Noa Yeshaya; Ashish Noronha; Moshit Lindzen; Emily K. Makowski; Ira Zaretsky; Yael Fridmann Sirkis; Yael Galon-Wolfenson; Peter M. Tessier; Jakub Abramson; Yosef Yarden; Deborah Fass; Sarel J. Fleishman

doi:10.1038/s41551-023-01079-1

Computational optimization of antibody humanness and stability by systematic energy-based ranking

Ariel Tennenhouse, Lev Khmelnitsky, Razi Khalaila, Noa Yeshaya, Ashish Noronha, Moshit Lindzen, Emily K. Makowski, Ira Zaretsky, Yael Fridmann Sirkis, Yael Galon-Wolfenson, Peter M. Tessier, Jakub Abramson, Yosef Yarden, Deborah Fass, Sarel J. Fleishman

Weizmann Institute of Science

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

Abstract

Conventional methods for humanizing animal-derived antibodies involve grafting their complementarity-determining regions onto homologous human framework regions. However, this process can substantially lower antibody stability and antigen-binding affinity, and requires iterative mutational fine-tuning to recover the original antibody properties. Here we report a computational method for the systematic grafting of animal complementarity-determining regions onto thousands of human frameworks. The method, which we named CUMAb (for computational human antibody design; available at http://CUMAb.weizmann.ac.il), starts from an experimental or model antibody structure and uses Rosetta atomistic simulations to select designs by energy and structural integrity. CUMAb-designed humanized versions of five antibodies exhibited similar affinities to those of the parental animal antibodies, with some designs showing marked improvement in stability. We also show that (1) non-homologous frameworks are often preferred to highest-homology frameworks, and (2) several CUMAb designs that differ by dozens of mutations and that use different human frameworks are functionally equivalent.

Original language	English
Pages (from-to)	30-44
Number of pages	15
Journal	Nature Biomedical Engineering
Volume	8
Issue number	1
Early online date	7 Aug 2023
DOIs	https://doi.org/10.1038/s41551-023-01079-1
State	Published - Jan 2024

All Science Journal Classification (ASJC) codes

Biotechnology
Bioengineering
Medicine (miscellaneous)
Biomedical Engineering
Computer Science Applications

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10.1038/s41551-023-01079-1

sjf_NatBiomedEngineering_ReliableEnergyBasedAntibody_AM2022Accepted author manuscript, 5.89 MBLicense: CC BY-NC-ND

https://doi.org/10.1101/2022.08.14.503891License: CC BY-NC-ND

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Tennenhouse, A., Khmelnitsky, L., Khalaila, R., Yeshaya, N., Noronha, A., Lindzen, M., Makowski, E. K., Zaretsky, I., Sirkis, Y. F., Galon-Wolfenson, Y., Tessier, P. M., Abramson, J., Yarden, Y., Fass, D., & Fleishman, S. J. (2024). Computational optimization of antibody humanness and stability by systematic energy-based ranking. Nature Biomedical Engineering, 8(1), 30-44. https://doi.org/10.1038/s41551-023-01079-1

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title = "Computational optimization of antibody humanness and stability by systematic energy-based ranking",

abstract = "Conventional methods for humanizing animal-derived antibodies involve grafting their complementarity-determining regions onto homologous human framework regions. However, this process can substantially lower antibody stability and antigen-binding affinity, and requires iterative mutational fine-tuning to recover the original antibody properties. Here we report a computational method for the systematic grafting of animal complementarity-determining regions onto thousands of human frameworks. The method, which we named CUMAb (for computational human antibody design; available at http://CUMAb.weizmann.ac.il), starts from an experimental or model antibody structure and uses Rosetta atomistic simulations to select designs by energy and structural integrity. CUMAb-designed humanized versions of five antibodies exhibited similar affinities to those of the parental animal antibodies, with some designs showing marked improvement in stability. We also show that (1) non-homologous frameworks are often preferred to highest-homology frameworks, and (2) several CUMAb designs that differ by dozens of mutations and that use different human frameworks are functionally equivalent.",

author = "Ariel Tennenhouse and Lev Khmelnitsky and Razi Khalaila and Noa Yeshaya and Ashish Noronha and Moshit Lindzen and Makowski, {Emily K.} and Ira Zaretsky and Sirkis, {Yael Fridmann} and Yael Galon-Wolfenson and Tessier, {Peter M.} and Jakub Abramson and Yosef Yarden and Deborah Fass and Fleishman, {Sarel J.}",

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doi = "10.1038/s41551-023-01079-1",

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Tennenhouse, A, Khmelnitsky, L, Khalaila, R, Yeshaya, N, Noronha, A, Lindzen, M, Makowski, EK, Zaretsky, I, Sirkis, YF, Galon-Wolfenson, Y, Tessier, PM, Abramson, J , Yarden, Y , Fass, D & Fleishman, SJ 2024, 'Computational optimization of antibody humanness and stability by systematic energy-based ranking', Nature Biomedical Engineering, vol. 8, no. 1, pp. 30-44. https://doi.org/10.1038/s41551-023-01079-1

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AU - Tennenhouse, Ariel

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AU - Noronha, Ashish

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AU - Makowski, Emily K.

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AU - Sirkis, Yael Fridmann

AU - Galon-Wolfenson, Yael

AU - Tessier, Peter M.

AU - Abramson, Jakub

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AU - Fass, Deborah

AU - Fleishman, Sarel J.

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Computational optimization of antibody humanness and stability by systematic energy-based ranking

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