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 -