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双膦酸盐偶联司帕沙星根除已建立的耐甲氧西林金黄色葡萄球菌感染并实现骨整合的证据:在植入物相关骨髓炎的小鼠模型中的研究。

Evidence of bisphosphonate-conjugated sitafloxacin eradication of established methicillin-resistant S. aureus infection with osseointegration in murine models of implant-associated osteomyelitis.

机构信息

Center for Musculoskeletal Research, University of Rochester Medical Center, Rochester, NY, 14642, USA.

Department of Orthopaedics, University of Rochester Medical Center, Rochester, NY, 14642, USA.

出版信息

Bone Res. 2023 Oct 18;11(1):51. doi: 10.1038/s41413-023-00287-4.

Abstract

Eradication of MRSA osteomyelitis requires elimination of distinct biofilms. To overcome this, we developed bisphosphonate-conjugated sitafloxacin (BCS, BV600072) and hydroxybisphosphonate-conjugate sitafloxacin (HBCS, BV63072), which achieve "target-and-release" drug delivery proximal to the bone infection and have prophylactic efficacy against MRSA static biofilm in vitro and in vivo. Here we evaluated their therapeutic efficacy in a murine 1-stage exchange femoral plate model with bioluminescent MRSA (USA300LAC::lux). Osteomyelitis was confirmed by CFU on the explants and longitudinal bioluminescent imaging (BLI) after debridement and implant exchange surgery on day 7, and mice were randomized into seven groups: 1) Baseline (harvested at day 7, no treatment); 2) HPBP (bisphosphonate control for BCS) + vancomycin; 3) HPHBP (hydroxybisphosphonate control for HBCS) + vancomycin; 4) vancomycin; 5) sitafloxacin; 6) BCS + vancomycin; and 7) HBCS + vancomycin. BLI confirmed infection persisted in all groups except for mice treated with BCS or HBCS + vancomycin. Radiology revealed catastrophic femur fractures in all groups except mice treated with BCS or HBCS + vancomycin, which also displayed decreases in peri-implant bone loss, osteoclast numbers, and biofilm. To confirm this, we assessed the efficacy of vancomycin, sitafloxacin, and HBCS monotherapy in a transtibial implant model. The results showed complete lack of vancomycin efficacy while all mice treated with HBCS had evidence of infection control, and some had evidence of osseous integrated septic implants, suggestive of biofilm eradication. Taken together these studies demonstrate that HBCS adjuvant with standard of care debridement and vancomycin therapy has the potential to eradicate MRSA osteomyelitis.

摘要

消除耐甲氧西林金黄色葡萄球菌(MRSA)骨髓炎需要消除不同的生物膜。为了克服这一问题,我们开发了双膦酸盐偶联司帕沙星(BCS,BV600072)和羟基亚膦酸盐偶联司帕沙星(HBCS,BV63072),它们能够在靠近骨感染的部位实现“靶向-释放”药物递送,并且在体外和体内对 MRSA 静态生物膜具有预防作用。在这里,我们在使用生物发光 MRSA(USA300LAC::lux)的 1 期交换股骨板模型中评估了它们的治疗效果。在清创和植入物交换手术后第 7 天,通过 CFU 对标本进行确认,并通过纵向生物发光成像(BLI)进行确认,然后将小鼠随机分为 7 组:1)基线(在第 7 天收获,未治疗);2)HPBP(BCS 的双膦酸盐对照物+万古霉素);3)HPHBP(HBCS 的羟基亚膦酸盐对照物+万古霉素);4)万古霉素;5)司帕沙星;6)BCS+万古霉素;7)HBCS+万古霉素。BLI 证实除了接受 BCS 或 HBCS+万古霉素治疗的小鼠外,所有组的感染均持续存在。放射学显示除了接受 BCS 或 HBCS+万古霉素治疗的小鼠外,所有组的股骨都发生了灾难性骨折,并且还显示出植入物周围骨丢失、破骨细胞数量和生物膜减少。为了证实这一点,我们评估了万古霉素、司帕沙星和 HBCS 单药治疗在胫骨植入模型中的疗效。结果表明,万古霉素完全无效,而所有接受 HBCS 治疗的小鼠均有感染控制的证据,有些小鼠有骨整合性感染植入物的证据,提示生物膜被清除。这些研究表明,HBCS 联合标准清创术和万古霉素治疗有可能根除 MRSA 骨髓炎。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca41/10582111/939b2d6eb6ea/41413_2023_287_Fig1_HTML.jpg

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