Yu M, Tomasa G
Department of Surgery, University of Hawaii, Honolulu 96813.
Crit Care Med. 1993 Nov;21(11):1635-42. doi: 10.1097/00003246-199311000-00010.
To determine if ketoconazole, a thromboxane A2 synthetase inhibitor, given within the first 24 hrs after diagnosis and arrival in the intensive care unit (ICU) would decrease the frequency of adult respiratory distress syndrome in the septic patient population.
Prospective, randomized, double-blind, placebo-controlled study.
Twelve-bed, surgical ICU in a university-affiliated hospital.
Fifty-four consecutive patients admitted to the surgical ICU with the diagnosis of sepsis composed the study sample. Sepsis was defined as including two or more of the following signs in a patient with a systolic blood pressure of < 80 mm Hg or a systemic vascular resistance of < 800 dyne.sec/cm5: a) temperature > or = 39 degrees C or < or = 35 degrees C; b) white blood cell count of > 12,000 leukocytes, or < or = 4000 leukocytes/microL, or > or = 20% immature cells; c) positive blood culture; d) known or strongly suspected source of infection from which a known pathogen was cultured.
Patients were randomized to receive either ketoconazole (400 mg) or placebo in a double-blind fashion as early as possible and in < 24 hrs after surgical ICU admission or after the diagnosis of sepsis was established.
Adult respiratory distress syndrome (ARDS) was diagnosed if the following criteria were met: a) intrapulmonary shunt of > 20%, or a PaO2/FIO2 ratio of < 150 requiring ventilatory support for > 48 hrs; b) pulmonary artery occlusion pressure of < 18 mm Hg and no clinical signs of heart failure; and c) diffuse infiltrates on chest radiograph. Treatment resulted in significant (p = .002) reduction in the frequency of ARDS compared with the placebo group, 64% vs. 15% in the ketoconazole treated group. The mortality rate was also reduced from 39% in the placebo group to 15% in the ketoconazole group (p = .05). A statistically significant reduction in ventilator and ICU days was not achieved.
Ketoconazole (400 mg through the gastrointestinal tract) given early in the septic course may prevent ARDS and decrease the mortality rate in high-risk, septic patients.
确定在诊断并入住重症监护病房(ICU)后的头24小时内给予血栓素A2合成酶抑制剂酮康唑,是否会降低脓毒症患者群体中成人呼吸窘迫综合征的发生率。
前瞻性、随机、双盲、安慰剂对照研究。
一所大学附属医院的拥有12张床位的外科ICU。
连续54例入住外科ICU且诊断为脓毒症的患者组成研究样本。脓毒症定义为收缩压<80mmHg或体循环血管阻力<800达因·秒/厘米⁵的患者出现以下两种或更多体征:a)体温≥39℃或≤35℃;b)白细胞计数>12,000/微升或≤4000/微升,或≥20%未成熟细胞;c)血培养阳性;d)已知或高度怀疑的感染源且培养出已知病原体。
患者被随机分组,尽早且在入住外科ICU后或脓毒症诊断确立后的24小时内,以双盲方式接受酮康唑(400毫克)或安慰剂治疗。
若符合以下标准,则诊断为成人呼吸窘迫综合征(ARDS):a)肺内分流>20%,或动脉血氧分压/吸入氧分数值(PaO2/FIO2)<150且需要机械通气支持>48小时;b)肺动脉楔压<18mmHg且无心力衰竭的临床体征;c)胸部X线片显示弥漫性浸润。与安慰剂组相比,治疗使ARDS发生率显著降低(p = 0.002),酮康唑治疗组为64%,安慰剂组为15%。死亡率也从安慰剂组的39%降至酮康唑组的15%(p = 0.05)。机械通气天数和ICU住院天数未实现统计学上的显著减少。
在脓毒症病程早期经胃肠道给予酮康唑(400毫克)可能预防ARDS并降低高危脓毒症患者的死亡率。
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