Banerjee Debolina, Feng Jun, Sellke Frank W
Division of Cardiothoracic Surgery, Department of Surgery, Brown University/Rhode Island Hospital, Providence, RI, United States.
Front Surg. 2024 Jul 3;11:1224068. doi: 10.3389/fsurg.2024.1224068. eCollection 2024.
Cardiopulmonary bypass (CPB) initiates an intense inflammatory response due to various factors: conversion from pulsatile to laminar flow, cold cardioplegia, surgical trauma, endotoxemia, ischemia-reperfusion injury, oxidative stress, hypothermia, and contact activation of cells by the extracorporeal circuit. Redundant and overlapping inflammatory cascades amplify the initial response to produce a systemic inflammatory response, heightened by coincident activation of coagulation and fibrinolytic pathways. When unchecked, this inflammatory response can become maladaptive and lead to serious postoperative complications. Concerted research efforts have been made to identify technical refinements and pharmacologic interventions that appropriately attenuate the inflammatory response and ultimately translate to improved clinical outcomes. Surface modification of the extracorporeal circuit to increase biocompatibility, miniaturized circuits with sheer resistance, filtration techniques, and minimally invasive approaches have improved clinical outcomes in specific populations. Pharmacologic adjuncts, including aprotinin, steroids, monoclonal antibodies, and free radical scavengers, show real promise. A multimodal approach incorporating technical, circuit-specific, and pharmacologic strategies will likely yield maximal clinical benefit.
体外循环(CPB)由于多种因素引发强烈的炎症反应:从搏动血流转变为层流、冷停搏液、手术创伤、内毒素血症、缺血-再灌注损伤、氧化应激、低温以及体外循环对细胞的接触激活。冗余且重叠的炎症级联反应放大了初始反应,通过凝血和纤溶途径的同时激活而加剧,从而产生全身炎症反应。如果不加控制,这种炎症反应可能会变得适应不良并导致严重的术后并发症。人们已经共同努力进行研究,以确定能够适当减轻炎症反应并最终转化为改善临床结果的技术改进和药物干预措施。体外循环的表面改性以提高生物相容性、具有剪切阻力的小型化回路、过滤技术以及微创方法已在特定人群中改善了临床结果。包括抑肽酶、类固醇、单克隆抗体和自由基清除剂在内的药物辅助手段显示出真正的前景。采用技术、回路特异性和药物策略的多模式方法可能会产生最大的临床益处。
