Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation

Pazhanichamy Kalailingam; So Fong Cam Ngan; Ranjith Iyappan; Afra Nehchiri; Khalilatul Hanisah Mohd-Kahliab; Benjamin Sian Teck Lee; Bhargy Sharma; Radek Machan; Sint Thida Bo; Emma S. Chambers; Val A. Fajardo; Rebecca E.K. Macpherson; Jian Liu; Panagiota Klentrou; Evangelia Litsa Tsiani; Kah Leong Lim; I. Hsin Su; Yong Gui Gao; A. Mark Richar; Raj N. Kalaria; Christopher P. Chen; Cynthia Balion; Dominique de Kleijn; Neil E. McCarthy; Siu Kwan Sze

doi:10.1111/acel.14425

Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation

Pazhanichamy Kalailingam^*, So Fong Cam Ngan, Ranjith Iyappan, Afra Nehchiri, Khalilatul Hanisah Mohd-Kahliab, Benjamin Sian Teck Lee, Bhargy Sharma, Radek Machan, Sint Thida Bo, Emma S. Chambers, Val A. Fajardo, Rebecca E.K. Macpherson, Jian Liu, Panagiota Klentrou, Evangelia Litsa Tsiani, Kah Leong Lim, I. Hsin Su, Yong Gui Gao, A. Mark Richar, Raj N. KalariaChristopher P. Chen, Cynthia Balion, Dominique de Kleijn, Neil E. McCarthy^*, Siu Kwan Sze^*

^*Corresponding author for this work

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

Abstract

Accumulation of damaged biomolecules in body tissues is the primary cause of aging and age-related chronic diseases. Since this damage often occurs spontaneously, it has traditionally been regarded as untreatable, with typical therapeutic strategies targeting genes or enzymes being ineffective in this domain. In this report, we demonstrate that an antibody targeting the isoDGR damage motif in lung tissue can guide immune clearance of harmful damaged proteins in vivo, effectively reducing age-linked lung inflammation. We observed age-dependent accumulation of the isoDGR motif in human lung tissues, as well as an 8-fold increase in isoDGR-damaged proteins in lung fibrotic tissues compared with healthy tissue. This increase was accompanied by marked infiltration of CD68+/CD11b + macrophages, consistent with a role for isoDGR in promoting chronic inflammation. We therefore assessed isoDGR function in mice that were either naturally aged or lacked the isoDGR repair enzyme. IsoDGR-protein accumulation in mouse lung tissue was strongly correlated with chronic inflammation, pulmonary edema, and hypoxemia. This accumulation also induced mitochondrial and ribosomal dysfunction, in addition to features of cellular senescence, thereby contributing to progressive lung damage over time. Importantly, treatment with anti-isoDGR antibody was able to reduce these molecular features of disease and significantly reduced lung pathology in vivo.

Original language	English
Article number	e14425
Journal	Aging Cell
Volume	24
Issue number	4
Early online date	5 Jan 2025
DOIs	https://doi.org/10.1111/acel.14425
Publication status	Published - Apr 2025

Keywords

antibody
immune clearance
immunotherapy
inflammation
isoDGR
lung fibrosis

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Aging Cell - 2025 - Kalailingam - Immunotherapeutic targeting of aging‐associated isoDGR motif in chronic lung inflammationFinal published version, 6.19 MBLicence: CC BY

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Kalailingam, P., Ngan, S. F. C., Iyappan, R., Nehchiri, A., Mohd-Kahliab, K. H., Lee, B. S. T., Sharma, B., Machan, R., Bo, S. T., Chambers, E. S., Fajardo, V. A., Macpherson, R. E. K., Liu, J., Klentrou, P., Tsiani, E. L., Lim, K. L., Su, I. H., Gao, Y. G., Richar, A. M., ... Sze, S. K. (2025). Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation. Aging Cell, 24(4), Article e14425. https://doi.org/10.1111/acel.14425

@article{c25f46d71e8644b2859aef898c6e67ab,

title = "Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation",

abstract = "Accumulation of damaged biomolecules in body tissues is the primary cause of aging and age-related chronic diseases. Since this damage often occurs spontaneously, it has traditionally been regarded as untreatable, with typical therapeutic strategies targeting genes or enzymes being ineffective in this domain. In this report, we demonstrate that an antibody targeting the isoDGR damage motif in lung tissue can guide immune clearance of harmful damaged proteins in vivo, effectively reducing age-linked lung inflammation. We observed age-dependent accumulation of the isoDGR motif in human lung tissues, as well as an 8-fold increase in isoDGR-damaged proteins in lung fibrotic tissues compared with healthy tissue. This increase was accompanied by marked infiltration of CD68+/CD11b + macrophages, consistent with a role for isoDGR in promoting chronic inflammation. We therefore assessed isoDGR function in mice that were either naturally aged or lacked the isoDGR repair enzyme. IsoDGR-protein accumulation in mouse lung tissue was strongly correlated with chronic inflammation, pulmonary edema, and hypoxemia. This accumulation also induced mitochondrial and ribosomal dysfunction, in addition to features of cellular senescence, thereby contributing to progressive lung damage over time. Importantly, treatment with anti-isoDGR antibody was able to reduce these molecular features of disease and significantly reduced lung pathology in vivo.",

keywords = "antibody, immune clearance, immunotherapy, inflammation, isoDGR, lung fibrosis",

author = "Pazhanichamy Kalailingam and Ngan, {So Fong Cam} and Ranjith Iyappan and Afra Nehchiri and Mohd-Kahliab, {Khalilatul Hanisah} and Lee, {Benjamin Sian Teck} and Bhargy Sharma and Radek Machan and Bo, {Sint Thida} and Chambers, {Emma S.} and Fajardo, {Val A.} and Macpherson, {Rebecca E.K.} and Jian Liu and Panagiota Klentrou and Tsiani, {Evangelia Litsa} and Lim, {Kah Leong} and Su, {I. Hsin} and Gao, {Yong Gui} and Richar, {A. Mark} and Kalaria, {Raj N.} and Chen, {Christopher P.} and Cynthia Balion and {de Kleijn}, Dominique and McCarthy, {Neil E.} and Sze, {Siu Kwan}",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s). Aging Cell published by Anatomical Society and John Wiley & Sons Ltd.",

year = "2025",

month = apr,

doi = "10.1111/acel.14425",

language = "English",

volume = "24",

journal = "Aging Cell",

issn = "1474-9718",

publisher = "Wiley-Blackwell",

number = "4",

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Kalailingam, P, Ngan, SFC, Iyappan, R, Nehchiri, A, Mohd-Kahliab, KH, Lee, BST, Sharma, B, Machan, R, Bo, ST, Chambers, ES, Fajardo, VA, Macpherson, REK, Liu, J, Klentrou, P, Tsiani, EL, Lim, KL, Su, IH, Gao, YG, Richar, AM, Kalaria, RN, Chen, CP, Balion, C, de Kleijn, D, McCarthy, NE & Sze, SK 2025, 'Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation', Aging Cell, vol. 24, no. 4, e14425. https://doi.org/10.1111/acel.14425

TY - JOUR

T1 - Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation

AU - Kalailingam, Pazhanichamy

AU - Ngan, So Fong Cam

AU - Iyappan, Ranjith

AU - Nehchiri, Afra

AU - Mohd-Kahliab, Khalilatul Hanisah

AU - Lee, Benjamin Sian Teck

AU - Sharma, Bhargy

AU - Machan, Radek

AU - Bo, Sint Thida

AU - Chambers, Emma S.

AU - Fajardo, Val A.

AU - Macpherson, Rebecca E.K.

AU - Liu, Jian

AU - Klentrou, Panagiota

AU - Tsiani, Evangelia Litsa

AU - Lim, Kah Leong

AU - Su, I. Hsin

AU - Gao, Yong Gui

AU - Richar, A. Mark

AU - Kalaria, Raj N.

AU - Chen, Christopher P.

AU - Balion, Cynthia

AU - de Kleijn, Dominique

AU - McCarthy, Neil E.

AU - Sze, Siu Kwan

PY - 2025/4

Y1 - 2025/4

N2 - Accumulation of damaged biomolecules in body tissues is the primary cause of aging and age-related chronic diseases. Since this damage often occurs spontaneously, it has traditionally been regarded as untreatable, with typical therapeutic strategies targeting genes or enzymes being ineffective in this domain. In this report, we demonstrate that an antibody targeting the isoDGR damage motif in lung tissue can guide immune clearance of harmful damaged proteins in vivo, effectively reducing age-linked lung inflammation. We observed age-dependent accumulation of the isoDGR motif in human lung tissues, as well as an 8-fold increase in isoDGR-damaged proteins in lung fibrotic tissues compared with healthy tissue. This increase was accompanied by marked infiltration of CD68+/CD11b + macrophages, consistent with a role for isoDGR in promoting chronic inflammation. We therefore assessed isoDGR function in mice that were either naturally aged or lacked the isoDGR repair enzyme. IsoDGR-protein accumulation in mouse lung tissue was strongly correlated with chronic inflammation, pulmonary edema, and hypoxemia. This accumulation also induced mitochondrial and ribosomal dysfunction, in addition to features of cellular senescence, thereby contributing to progressive lung damage over time. Importantly, treatment with anti-isoDGR antibody was able to reduce these molecular features of disease and significantly reduced lung pathology in vivo.

AB - Accumulation of damaged biomolecules in body tissues is the primary cause of aging and age-related chronic diseases. Since this damage often occurs spontaneously, it has traditionally been regarded as untreatable, with typical therapeutic strategies targeting genes or enzymes being ineffective in this domain. In this report, we demonstrate that an antibody targeting the isoDGR damage motif in lung tissue can guide immune clearance of harmful damaged proteins in vivo, effectively reducing age-linked lung inflammation. We observed age-dependent accumulation of the isoDGR motif in human lung tissues, as well as an 8-fold increase in isoDGR-damaged proteins in lung fibrotic tissues compared with healthy tissue. This increase was accompanied by marked infiltration of CD68+/CD11b + macrophages, consistent with a role for isoDGR in promoting chronic inflammation. We therefore assessed isoDGR function in mice that were either naturally aged or lacked the isoDGR repair enzyme. IsoDGR-protein accumulation in mouse lung tissue was strongly correlated with chronic inflammation, pulmonary edema, and hypoxemia. This accumulation also induced mitochondrial and ribosomal dysfunction, in addition to features of cellular senescence, thereby contributing to progressive lung damage over time. Importantly, treatment with anti-isoDGR antibody was able to reduce these molecular features of disease and significantly reduced lung pathology in vivo.

KW - antibody

KW - immune clearance

KW - immunotherapy

KW - inflammation

KW - isoDGR

KW - lung fibrosis

UR - http://www.scopus.com/inward/record.url?scp=85214141040&partnerID=8YFLogxK

U2 - 10.1111/acel.14425

DO - 10.1111/acel.14425

M3 - Article

C2 - 39757428

AN - SCOPUS:85214141040

SN - 1474-9718

VL - 24

JO - Aging Cell

JF - Aging Cell

IS - 4

M1 - e14425

ER -

Immunotherapeutic targeting of aging-associated isoDGR motif in chronic lung inflammation

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