Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences

Danyang Zhao; Chao Han; Elmina Mammadova-Bach; Kanako Watanabe-Kusunoki; Tamisa Seeko Bandeira Honda; Yihong Li; Chenyu Li; Qiubo Li; Hao Long; Lyuben Lyubenov; Chongxu Shi; Donato Santovito; Christian Weber; Peter Boor; Patrick Droste; Samir Parikh; John Shapiro; Letizia De Chiara; Giulia Carangelo; Paola Romagnani; Sven Klussmann; Axel Vater; Hans-Joachim Anders

doi:10.1016/j.kint.2024.07.020

Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences

Danyang Zhao
, Chao Han
, Elmina Mammadova-Bach
, Kanako Watanabe-Kusunoki
, Tamisa Seeko Bandeira Honda
, Yihong Li
, Chenyu Li
, Qiubo Li
, Hao Long
, Lyuben Lyubenov
, Chongxu Shi
, Donato Santovito
, Christian Weber
, Peter Boor
, Patrick Droste
, Samir Parikh
, John Shapiro
, Letizia De Chiara
, Giulia Carangelo
, Paola Romagnani

Sven Klussmann, Axel Vater, Hans-Joachim Anders^*

^*Corresponding author for this work

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

Abstract

Cholesterol crystal embolism (CCE) implies immunothrombosis, tissue necrosis, and organ failure but no specific treatments are available. As CCE involves complement activation, we speculated that inhibitors of the C5a/C5aR axis would be sufficient to attenuate the consequences of CCE like that with systemic vasculitis. Cholesterol microcrystal injection into the kidney artery of wildtype mice initiated intra-kidney immunothrombosis within a few hours followed by a sudden drop of glomerular filtration rate and ischemic kidney necrosis after 24 hours. Genetic deficiency of either C3 or C5aR prevented immunothrombosis, glomerular filtration rate drop, and ischemic necrosis at 24 hours as did preemptive treatment with inhibitors of either C5a or C5aR. Delayed C5a blockade after crystal injection still resolved crystal clots and prevented all consequences. Thus, selective blockade of C5a or C5aR is sufficient to attenuate the consequences of established CCE and prospective inhibition in high-risk patients may be clinically feasible and safe.

Original language	English
Pages (from-to)	819-825
Number of pages	7
Journal	Kidney International
Volume	106
Issue number	5
Early online date	12 Aug 2024
DOIs	https://doi.org/10.1016/j.kint.2024.07.020
Publication status	Published - Nov 2024

Keywords

acute kidney injury
diabetes
infarct
necroinflammation
thrombosis

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Zhao, D., Han, C., Mammadova-Bach, E., Watanabe-Kusunoki, K., Bandeira Honda, T. S., Li, Y., Li, C., Li, Q., Long, H., Lyubenov, L., Shi, C., Santovito, D., Weber, C., Boor, P., Droste, P., Parikh, S., Shapiro, J., De Chiara, L., Carangelo, G., ... Anders, H.-J. (2024). Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences. Kidney International, 106(5), 819-825. https://doi.org/10.1016/j.kint.2024.07.020

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title = "Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences",

abstract = "Cholesterol crystal embolism (CCE) implies immunothrombosis, tissue necrosis, and organ failure but no specific treatments are available. As CCE involves complement activation, we speculated that inhibitors of the C5a/C5aR axis would be sufficient to attenuate the consequences of CCE like that with systemic vasculitis. Cholesterol microcrystal injection into the kidney artery of wildtype mice initiated intra-kidney immunothrombosis within a few hours followed by a sudden drop of glomerular filtration rate and ischemic kidney necrosis after 24 hours. Genetic deficiency of either C3 or C5aR prevented immunothrombosis, glomerular filtration rate drop, and ischemic necrosis at 24 hours as did preemptive treatment with inhibitors of either C5a or C5aR. Delayed C5a blockade after crystal injection still resolved crystal clots and prevented all consequences. Thus, selective blockade of C5a or C5aR is sufficient to attenuate the consequences of established CCE and prospective inhibition in high-risk patients may be clinically feasible and safe.",

keywords = "acute kidney injury, diabetes, infarct, necroinflammation, thrombosis",

author = "Danyang Zhao and Chao Han and Elmina Mammadova-Bach and Kanako Watanabe-Kusunoki and \{Bandeira Honda\}, \{Tamisa Seeko\} and Yihong Li and Chenyu Li and Qiubo Li and Hao Long and Lyuben Lyubenov and Chongxu Shi and Donato Santovito and Christian Weber and Peter Boor and Patrick Droste and Samir Parikh and John Shapiro and \{De Chiara\}, Letizia and Giulia Carangelo and Paola Romagnani and Sven Klussmann and Axel Vater and Hans-Joachim Anders",

year = "2024",

month = nov,

doi = "10.1016/j.kint.2024.07.020",

language = "English",

volume = "106",

pages = "819--825",

journal = "Kidney International",

issn = "0085-2538",

publisher = "Elsevier B.V.",

number = "5",

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Zhao, D, Han, C, Mammadova-Bach, E, Watanabe-Kusunoki, K, Bandeira Honda, TS, Li, Y, Li, C, Li, Q, Long, H, Lyubenov, L, Shi, C, Santovito, D, Weber, C, Boor, P, Droste, P, Parikh, S, Shapiro, J, De Chiara, L, Carangelo, G, Romagnani, P, Klussmann, S, Vater, A & Anders, H-J 2024, 'Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences', Kidney International, vol. 106, no. 5, pp. 819-825. https://doi.org/10.1016/j.kint.2024.07.020

TY - JOUR

T1 - Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences

AU - Zhao, Danyang

AU - Han, Chao

AU - Mammadova-Bach, Elmina

AU - Watanabe-Kusunoki, Kanako

AU - Bandeira Honda, Tamisa Seeko

AU - Li, Yihong

AU - Li, Chenyu

AU - Li, Qiubo

AU - Long, Hao

AU - Lyubenov, Lyuben

AU - Shi, Chongxu

AU - Santovito, Donato

AU - Weber, Christian

AU - Boor, Peter

AU - Droste, Patrick

AU - Parikh, Samir

AU - Shapiro, John

AU - De Chiara, Letizia

AU - Carangelo, Giulia

AU - Romagnani, Paola

AU - Klussmann, Sven

AU - Vater, Axel

AU - Anders, Hans-Joachim

PY - 2024/11

Y1 - 2024/11

N2 - Cholesterol crystal embolism (CCE) implies immunothrombosis, tissue necrosis, and organ failure but no specific treatments are available. As CCE involves complement activation, we speculated that inhibitors of the C5a/C5aR axis would be sufficient to attenuate the consequences of CCE like that with systemic vasculitis. Cholesterol microcrystal injection into the kidney artery of wildtype mice initiated intra-kidney immunothrombosis within a few hours followed by a sudden drop of glomerular filtration rate and ischemic kidney necrosis after 24 hours. Genetic deficiency of either C3 or C5aR prevented immunothrombosis, glomerular filtration rate drop, and ischemic necrosis at 24 hours as did preemptive treatment with inhibitors of either C5a or C5aR. Delayed C5a blockade after crystal injection still resolved crystal clots and prevented all consequences. Thus, selective blockade of C5a or C5aR is sufficient to attenuate the consequences of established CCE and prospective inhibition in high-risk patients may be clinically feasible and safe.

AB - Cholesterol crystal embolism (CCE) implies immunothrombosis, tissue necrosis, and organ failure but no specific treatments are available. As CCE involves complement activation, we speculated that inhibitors of the C5a/C5aR axis would be sufficient to attenuate the consequences of CCE like that with systemic vasculitis. Cholesterol microcrystal injection into the kidney artery of wildtype mice initiated intra-kidney immunothrombosis within a few hours followed by a sudden drop of glomerular filtration rate and ischemic kidney necrosis after 24 hours. Genetic deficiency of either C3 or C5aR prevented immunothrombosis, glomerular filtration rate drop, and ischemic necrosis at 24 hours as did preemptive treatment with inhibitors of either C5a or C5aR. Delayed C5a blockade after crystal injection still resolved crystal clots and prevented all consequences. Thus, selective blockade of C5a or C5aR is sufficient to attenuate the consequences of established CCE and prospective inhibition in high-risk patients may be clinically feasible and safe.

KW - acute kidney injury

KW - diabetes

KW - infarct

KW - necroinflammation

KW - thrombosis

U2 - 10.1016/j.kint.2024.07.020

DO - 10.1016/j.kint.2024.07.020

M3 - Article

SN - 0085-2538

VL - 106

SP - 819

EP - 825

JO - Kidney International

JF - Kidney International

IS - 5

ER -

Inhibition of complement factor C5a or C5aR for cholesterol crystal embolism-related vascular thrombosis with microvascular injury and its consequences

Abstract

Keywords

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