Complement activation and neutrophil stimulation are two major components in events leading to ischemia and reperfusion (IR) injury. C1 inhibitor (C1INH) inhibits activation of each of the three pathways of complement activation and of the contact system. It is also endowed with anti-inflammatory properties that are independent of protease inhibition. The goal of these studies was to investigate the role and mechanism of C1INH in alleviating IR-induced intestinal injury. C57BL/6, C1INH-deficient (C1INH(-/-)), bradykinin type 2 receptor-deficient (Bk2R(-/-)), and C3-deficient mice (C3(-/-)) were randomized into three groups: sham operated control, IR, and IR + C1INH-treated groups. Ischemia was generated by occlusion of the superior mesenteric artery followed by reperfusion. C1INH or reactive center-cleaved inactive C1INH (iC1INH) was injected intravenously before reperfusion. IR resulted in intestinal injury in C57BL/6, C1INH(-/-), Bk2R(-/-), and C3(-/-) mice with significantly increased neutrophil infiltration into intestinal tissue. In each mouse strain, C1INH treatment reduced intestinal tissue injury and attenuated leukocyte infiltration compared with the untreated IR group. C1INH inhibited leukocyte rolling in the mesenteric veins of both C57BL/6 and C3-deficient mice subjected to IR. C1INH treatment also improved the survival rate of C57BL/6 and C1INH(-/-) mice following IR. Similar findings were observed in the IR animals treated with iC1INH. These studies emphasize the therapeutic benefit of C1INH in preventing intestinal injury caused by IR. In addition to the protective activities mediated via inhibition of the complement system, these studies indicate that C1INH also plays a direct role in suppression of leukocyte transmigration into reperfused tissue.
机构:
CHU Poitiers, Serv Biochim, Poitiers, France
Univ Poitiers, Fac Med & Pharm, Poitiers, France
INSERM, U1082, Poitiers, FranceCHU Poitiers, Serv Biochim, Poitiers, France
Thuillier, R.
Lepape, S.
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Univ Poitiers, Fac Med & Pharm, Poitiers, France
INSERM, U1082, Poitiers, FranceCHU Poitiers, Serv Biochim, Poitiers, France
Lepape, S.
Saintyves, T.
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INSERM, U1082, Poitiers, FranceCHU Poitiers, Serv Biochim, Poitiers, France
Saintyves, T.
Danion, J.
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INSERM, U1082, Poitiers, FranceCHU Poitiers, Serv Biochim, Poitiers, France
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Saglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Sogukpinar, I. Cenk
Sahin, Duygu
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Gazi Univ, Tibbi Biyokimya Anabilim Dali, Tip Fak, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Sahin, Duygu
Demirag, Alp
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Yeditepe Univ, Hastanesi Genel Cerrahi, Istanbul, Turkey
Yeditepe Univ, Organ Nakli AD, Istanbul, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Demirag, Alp
Sepici-Dincel, Aylin
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Gazi Univ, Tibbi Biyokimya Anabilim Dali, Tip Fak, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Sepici-Dincel, Aylin
Kisakurek, Mustafa
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Saglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Kisakurek, Mustafa
Akkus, M. Ali
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Saglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey
Akkus, M. Ali
Altan, Nilguen
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Gazi Univ, Tibbi Biyokimya Anabilim Dali, Tip Fak, Ankara, TurkeySaglik Bakanligi Ankara Egitim & Arastirma Hastan, Genel Cerrahi Klin, Ankara, Turkey