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Merck

Developing dual hemofiltration plus cardiopulmonary bypass in rodents.

The Journal of surgical research (2015-01-04)
Koichiro Shinozaki, Joshua W Lampe, Chih-Hsien Wang, Tai Yin, Junhwan Kim, Shigeto Oda, Hiroyuki Hirasawa, Lance B Becker
摘要

Emerging therapies for prolonged cardiac arrest (CA) include advanced circulatory interventions like emergency cardiopulmonary bypass (ECPB) and continuous venovenous hemofiltration (CVVHF). However, preclinical studies are limited because of the absence of a practical method of using CVVHF along with ECPB in rodents. We modified a CA model with ECPB resuscitation to include the CVVHF circuit. Adult rats were cannulated via the femoral artery or vein and the jugular vein for the ECPB circuit. A new circuit for CVVHF was added to allow ECPB and CVVHF to be started simultaneously. CVVHF blood flow at 3 mL/min could be controlled with a screw clamp during ECPB. After cessation of ECPB, the CVVHF flow was maintained using a roller pump. The filtration rate was controlled at 40 mL/h/kg in the standard volume of CVVHF and 120 mL/h/kg in the high volume (HV) of CVVHF. The driving force of hemofiltration was evaluated by monitoring transmembrane pressure and filter clearance (FCL). Transmembrane pressure in both groups was stable for 6 h throughout CVVHF. FCL of blood urea nitrogen and potassium in the standard volume group was significantly less than the HV group (P < 0.01). FCL of blood urea nitrogen and potassium was stable throughout the CVVHF operation in both groups. We developed a method of CVVHF along with ECPB in rodents after CA. We further demonstrated the ability to regulate both standard and HV filtration rates.

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钾, chunks (in mineral oil), 98% trace metals basis
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氢化钾, 30 wt % dispersion in mineral oil
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氢化钾, in paraffin
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维库溴铵
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维库溴铵, United States Pharmacopeia (USP) Reference Standard
维库溴铵, European Pharmacopoeia (EP) Reference Standard