作者
Allison Bauman,Jansy P. Sarathy,Firat Kaya,Lisa M. Massoudi,Michael S. Scherman,Courtney Hastings,Jiuyu Liu,Min Xie,Elizabeth J. Brooks,Michelle E. Ramey,Isabelle L. Jones,Noalani D. Benedict,Madelyn R. Maclaughlin,Jake A. Miller-Dawson,Samanthi L. Waidyarachchi,Michelle M. Butler,Terry L. Bowlin,Matthew Zimmerman,Anne J. Lenaerts,Bernd Meibohm,Mercedes Gonzalez‐Juarrero,Michael A. Lyons,Véronique Dartois,Richard Lee,Gregory T. Robertson
摘要
ABSTRACT The spectinamides are novel, narrow-spectrum semisynthetic analogs of spectinomycin, modified to avoid intrinsic efflux by Mycobacterium tuberculosis . Spectinamides, including lead MBX-4888A (Lee-1810), exhibit promising therapeutic profiles in mice, as single drugs and as partner agents with other anti-tuberculosis antibiotics including rifampin and/or pyrazinamide. Here, we show that MBX-4888A, given by injection with the front-line standard of care regimen, is treatment shortening in multiple murine tuberculosis infection models. The positive treatment responses to MBX-4888A combination therapy in multiple mouse models, including mice exhibiting advanced pulmonary disease, can be attributed to favorable distribution in tissues and lesions, retention in caseum, along with favorable effects with rifampin and pyrazinamide under conditions achieved in necrotic lesions. This study also provides an additional data point regarding the safety and tolerability of spectinamide MBX-4888A in long-term murine efficacy studies.