Sheoran Abhineet S, Chapman-Bonofiglio Susan, Harvey Barrett R, Mukherjee Jean, Georgiou George, Donohue-Rolfe Arthur, Tzipori Saul
Tufts University School of Veterinary Medicine, Division of Infectious Diseases, 200 Westboro Rd., Building 20, North Grafton, MA 01536, USA.
Infect Immun. 2005 Aug;73(8):4607-13. doi: 10.1128/IAI.73.8.4607-4613.2005.
Infection of children with Shiga toxin (Stx)-producing Escherichia coli (STEC) can lead to hemolytic-uremic syndrome (HUS) in 5 to 10% of patients. Stx2, one of two toxins liberated by the bacterium, is directly linked with HUS. We have previously shown that Stx-specific human monoclonal antibodies protect STEC-infected animals from fatal systemic complications. The present study defines the protective antibody dose in relation to the time of treatment after the onset of diarrhea in infected gnotobiotic piglets. Using the mouse toxicity model, we selected 5C12, an antibody specific for the A subunit, as the most effective Stx2 antibody for further characterization in the piglet model in which piglets developed diarrhea 16 to 40 h after bacterial challenge, followed by fatal neurological symptoms at 48 to 96 h. Seven groups of piglets received doses of 5C12 ranging from 6.0 mg/kg to 0.05 mg/kg of body weight, administered parenterally 48 h after bacterial challenge. The minimum fully protective antibody dose was 0.4 mg/kg, and the corresponding serum antibody concentration in these piglets was 0.7 mug (+/-0.5)/ml, measured 7 to 14 days after administration. Of 40 infected animals which received Stx2 antibody treatment of > or =0.4 mg/kg, 34 (85%) survived, while only 1 (2.5%) of 39 placebo-treated animals survived. We conclude that the administration of the Stx2-specific antibody was protective against fatal systemic complications even when it was administered well after the onset of diarrhea. These findings suggest that children treated with this antibody, even after the onset of bloody diarrhea, may be equally protected against the risk of developing HUS.
感染产志贺毒素(Stx)的大肠杆菌(STEC)的儿童中,5%至10%的患者会发展为溶血尿毒综合征(HUS)。该细菌释放的两种毒素之一Stx2与HUS直接相关。我们之前已表明,Stx特异性人单克隆抗体可保护受STEC感染的动物免受致命的全身并发症。本研究确定了在感染的无菌仔猪腹泻发作后治疗时间与保护性抗体剂量的关系。使用小鼠毒性模型,我们选择了对A亚基特异的抗体5C12,作为最有效的Stx2抗体,在仔猪模型中进一步表征。在该模型中,仔猪在细菌攻击后16至40小时出现腹泻,随后在48至96小时出现致命的神经症状。七组仔猪接受了体重范围为6.0mg/kg至0.05mg/kg的5C12剂量,在细菌攻击后48小时经肠胃外给药。最小完全保护抗体剂量为0.4mg/kg,给药后7至14天测量,这些仔猪相应的血清抗体浓度为0.7μg(±0.5)/ml。接受≥0.4mg/kg Stx2抗体治疗的40只感染动物中,34只(85%)存活,而39只接受安慰剂治疗的动物中只有1只(2.5%)存活。我们得出结论,即使在腹泻发作后很久才给药,给予Stx2特异性抗体仍可预防致命的全身并发症。这些发现表明,即使在血性腹泻发作后用这种抗体治疗的儿童,也可能同样受到保护,避免发展为HUS的风险。
