In Australia, resistance to β-lactam-class antibiotics in Enterobacterales has increased. This study aimed to identify potential oral treatments for these multidrug-resistant infections by investigating four β-lactam (mecillinam, tebipenem, sulopenem, and faropenem) and three non-β-lactam (fosfomycin, omadacycline, and delafloxacin) antibiotics, and to elucidate the genetic resistance mechanisms.

METHODS:

Seventy-four Escherichia coli and 24 Klebsiella pneumoniae, with extended-spectrum β-lactamase or plasmid-mediated AmpC β-lactamases genes, were isolated from New South Wales hospital patients in 2021. Minimum inhibitory concentrations (MICs) were determined using Clinical and Laboratory Standards Institute (CLSI) guidelines with agar dilution for fosfomycin and mecillinam, and broth microdilution for the remaining antibiotics. Multiplex polymerase chain reaction and whole genome sequencing (Illumina) confirmed bacterial resistance mechanisms.

RESULTS:

The E. coli were mostly susceptible to mecillinam (97%), and had low MIC₉₀ to tebipenem, sulopenem, and faropenem (0.125 mg/L, 0.5 mg/L, and 4 mg/L). K. pneumoniae were mostly susceptible to mecillinam (96%), and had a low MIC₉₀ to tebipenem and sulopenem, but higher MIC₉₀ to faropenem (2 mg/L, 2 mg/L, and 8 mg/L). Moreover, the cases of E. coli were mostly susceptible to fosfomycin and omadacycline, but not delafloxacin (100%, 95%, and 16%); K. pneumoniae susceptibilities to these antibiotics were 92%, 50%, and 17%, respectively. Resistance mechanisms include tet(A) and ramR mutations for omadacycline; gyrA, parC, and qnr mutations for delafloxacin; and ompK36 gene deletions for fosfomycin, mecillinam, tebipenem, sulopenem, and faropenem.

CONCLUSIONS:

The favourable results support the use of mecillinam, tebipenem, sulopenem, faropenem, fosfomycin, and omadacycline against multidrug-resistant E. coli. Mecillinam, sulopenem, and fosfomycin may be useful for multidrug-resistant K. pneumoniae in Australia.

2025-08-01·ANNALS OF PHARMACOTHERAPY

Pivmecillinam for Uncomplicated Acute Cystitis: A Contemporary Review

Review

作者: White, Bryan P. ; Burchette, Jessica E. ; Covert, Kelly ; Chastain, Daniel B. ; Tu, Patrick ; Cluck, David B.

Objective::

To review the evidence and discuss use of pivmecillinam in uncomplicated acute cystitis.

Data sources::

A literature search was conducted utilizing PubMed (from 2000 through August 2024) and ClinicalTrials.gov. Medical Subject Headings (MeSH) terms, such as mecillinam or pivmecillinam and urinary tract infections, were utilized. Additional references were identified by reviewing literature citations.

Study selection and data extraction::

Articles were limited to English language publications evaluating the efficacy or safety of pivmecillinam for urinary tract infections (UTIs) in adult populations.

Data synthesis::

Data from 6 randomized controlled trials support pivmecillinam for acute uncomplicated cystitis at doses of 200 to 400 mg 3 times daily for 3 to 7 days, with more consistent clinical and bacteriologic cure observed with 400 mg doses and longer therapy durations. Clinical evaluation of 400 mg 2 to 3 times daily is available with use more common in non–US Food and Drug Administration (FDA)-approved populations, such as men, pregnancy, and multidrug resistant infections. There are limited data supporting pivmecillinam for pyelonephritis; routine use is cautioned until further clinical data are available.

Relevance to patient care and clinical practice in comparison with existing drugs::

As resistance to first-line antimicrobials rises, the need for safe and effective treatment options remains high. Pivmecillinam represents a new therapeutic option available in the United States for outpatient management of uncomplicated acute cystitis.

Conclusion::

Pivmecillinam could be a key agent for uncomplicated acute cystitis. Utilization will likely be cost driven, but the promise of low resistance encourages the place in therapy when other agents are not susceptible to infecting uropathogens.

2025-07-02·AMERICAN JOURNAL OF TROPICAL MEDICINE AND HYGIENE

Multidrug-Resistant Escherichia coli Isolated from Stool Samples of Healthy Infants in Rural Bangladeshi Communities

Article

作者: Ahmed, Tahmeed ; Ali, Hasmot ; Chakraborty, Subhra ; Labrique, Alain ; Hossain, Talal ; Islam, Riajul ; Rahman, Hafizur ; Palmer, Amanda C. ; Shaikh, Saijuddin ; Biswas, Sahitya Ranjan ; Johura, Fatema-Tuz ; Tasnim, Jarin ; Hossain, Md Iqbal ; Alam, Munirul

ABSTRACT.:

Escherichia coli (E. coli) is a commensal organism in humans and animals. It can serve as a reservoir for antibiotic resistance, thus providing an indicator of drug resistance patterns in a community. We investigated antibiotic resistance in E. coli isolated from nondiarrheal stool samples of 6-month-old infants (n = 110) from northwest Bangladesh. We conducted susceptibility testing using a disc diffusion assay against 20 antibiotics. Resistance was most pronounced for macrolides (98.2% resistant), whereas the most sensitive antibiotics were fosfomycin (100%), gentamicin (99.1%), meropenem (98.2%), mecillinam (97.3%), tigecycline (97.3%), and imipenem (87.3%). Excluding erythromycin, roughly 55% of isolates were multidrug-resistant. Our results likely reflect the burden of drug-resistant E. coli in the guts of infants in rural Bangladesh and the prevailing drug resistance patterns in this community.

项与美西林相关的新闻（医药）

2024-04-25

·FiercePharma

Utility Therapeutics wins FDA nod for UTI antibiotic that has been on the market in Europe for 40-plus years

Nearly half of women will get a urinary tract infection in their lifetime. For the first time in more than 20 years the FDA has approved an antibiotic to treat the condition. For the first time in more than 20 years, the FDA has approved a treatment for uncomplicated urinary tract infections (uUTI). And the nod has come for an oral antibiotic that has been available in Europe for more than 40 years. It’s an odd set of circumstances and a dose of foresight by Utility Therapeutics that bring Pivya (pivmecillinam) to the market in the United States in the therapy’s golden years. The London-based company was formed specifically to develop and commercialize pivmecillinam in the U.S. where antimicrobial resistance is growing to standard of care antibiotics. The decreased “utility” of first-line antibiotics and the void the company is attempting to fill in the U.S. were the inspiration of the name of the company. And the void is significant as more than 30 million uUTIs are diagnosed every year in the U.S., with nearly half of all women contracting the infection at some point in their life. Outside of hospital setting, UTIs account for more antibiotic use than any other disorder. In 2018, Utility inked a licensing agreement with LEO Pharma, acquiring the U.S. rights to pivmecillinam and its subcutaneous formulation mecillinam, which the company has submitted for approval as a first-line therapy for complicated urinary tract infections (cUTI) in the hospital setting. The difference between cUTIs and uUTIs is that the former has reached the kidneys while the latter is limited to the bladder. “The FDA is committed to fostering new antibiotic availability when they prove to be safe and effective and Pivya will provide an additional treatment option for uncomplicated UTIs,” Peter Kim, M.D., the director of the Division of Anti-Infectives at the FDA’s Center for Drug Evaluation and Research, said in a release. The year that Utility acquired the rights to pivmecillinam and mecillinam, the FDA signed off on each as a Qualified Infectious Disease Product (QIDP). The status is extended to antibacterial and antifungal drug candidates intended to treat serious or life-threatening infections. When a QIDP treatment is approved, it gains an additional five years of market exclusivity. On the same day in January, when Utility revealed that the FDA had accepted the company’s new drug applications for pivmecillinam and mecillinam, it also announced it had received private funding from the AMR Action Fund. The global initiative—which was established by several prominent drugmakers including Amgen, Bayer, Eli Lilly, GSK, Novo Nordisk and Roche—invests in the development of new antimicrobial therapeutics. In addition to being a prodrug, which means that it is not pharmacologically active until it is digested and absorbed into the system, Pivya has a unique mechanism of action, targeting penicillin binding protein-2 in the cell wall of gram-negative bacteria. Pivya’s efficacy was assessed in separate trials versus placebo, an oral antibacterial and ibuprofen. The primary measure of efficacy in the studies was the composite response rate, which included clinical cure (resolution of the symptoms of the uUTI that were present in patients at trial entry and no new symptoms) and microbiological response (demonstration that the bacteria cultured from patients’ urine at trial entry was reduced). In the placebo trial, 62% of the participants who received Pivya achieved composite response compared to 10% of those on placebo. In the oral antibacterial trial, 72% of the subjects who received Pivya achieved composite response versus 76% of those on the comparator. In the third trial, 66% of the subjects who received Pivya achieved composite response compared to 22% of those on ibuprofen. Commonly prescribed drugs for uUTIs in the U.S. are bactrim (sulphamethoxazole/trimethoprim), nitrofuranatoin and fluoroquinolones. But more than 1 in 5 who receive these are resistant, which can lead to progression of the disease, including life-threatening sepsis. Last month, Germany’s Allecra Therapeutics scored FDA approval for its antibiotic Exblifep, which is a combination of cephalosporin antibacterial cefepime and the beta-lactamase inhibitor enmetazobactam, to treat cUTI. The approval came days after the U.S. regulator rejected another combo therapy in the same indication from Venatorx Pharmaceuticals and Melinta Therapeutics.

引进/卖出上市批准临床结果

2024-04-24

·药明康德

半数女性一生中会罹患这类疾病……FDA今日批准应对手段

▎药明康德内容团队编辑今天，美国FDA宣布批准Utility Therapeutics开发的Pivya（pivmecillinam）片剂，用于治疗由大肠杆菌、奇异变形杆菌和腐生葡萄球菌的敏感分离株所引起的非复杂性尿路感染（UTI）女性成年患者。非复杂性尿路感染是指女性的膀胱受到细菌感染，但尿道结构并无异常。据研究，约有一半的女性一生中至少会经历一次尿路感染。Pivya用于治疗18岁及以上非复杂性尿路感染女性患者的疗效在三项对照临床试验中进行了评估，这些试验将不同的Pivya给药方案与安慰剂、另一种口服抗菌药物及ibuprofen（一种抗炎药物）进行了比较。三项试验的主要疗效评估指标为复合应答率，包括临床治愈（即试验入组时存在的非复杂性尿路感染症状得到缓解且无新症状出现）和微生物学应答（证明与入组时相较，患者尿液中培养的细菌减少）。复合应答率在患者入组后约8至14天进行评估。在与安慰剂比较的临床试验中，接受Pivya治疗的137名受试者中有62%达到了复合应答，而接受安慰剂的134名受试者中有10%达到此应答标准。在与另一种口服抗菌药物比较的临床试验中，接受Pivya治疗的127名受试者中有72%达到复合应答，而接受对照药物的132名受试者中有76%达到此应答标准。在与抗炎药物比较的临床试验中，接受Pivya治疗的105名受试者中有66%达到复合应答，而接受对照抗炎药物的119名受试者中有22%达到此应答标准。Pivya最常见的副作用包括恶心和腹泻。图片来源：123RFPivmecillinam是一种具有独特作用机制的β-内酰胺抗生素，过去40多年里，它已经在多个国家和地区用于治疗尿路感染。在体外和体内研究中，它表现出针对尿路感染中最常见细菌的活性，包括耐药性菌株。今年1月，Utility Therapeutics公司宣布美国FDA已经授予pivmecillinam的新药申请优先审评资格，用于治疗非复杂性尿路感染。Pivmecillinam和它的静脉注射剂型mecillinam均已获得FDA授予的合格传染病产品资格。了解更多FDA获批新药请点击下图访问我们的小程序▲欲了解更多前沿技术在生物医药产业中的应用，请长按扫描上方二维码，即可访问“药明直播间”，观看相关话题的直播讨论与精彩回放参考资料：[1] FDA Approves New Treatment for Uncomplicated Urinary Tract Infections. Retrieved April 24, 2024 from https://www.prnewswire.com/news-releases/fda-approves-new-treatment-for-uncomplicated-urinary-tract-infections-302126509.html免责声明：药明康德内容团队专注介绍全球生物医药健康研究进展。本文仅作信息交流之目的，文中观点不代表药明康德立场，亦不代表药明康德支持或反对文中观点。本文也不是治疗方案推荐。如需获得治疗方案指导，请前往正规医院就诊。版权说明：本文来自药明康德内容团队，欢迎个人转发至朋友圈，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载授权请在「药明康德」微信公众号回复“转载”，获取转载须知。分享，点赞，在看，聚焦全球生物医药健康创新

优先审批微生物疗法突破性疗法快速通道申请上市

2024-03-31

·药明康德

4月8款创新药有望获FDA批准

▎药明康德内容团队编辑根据PDUFA的预期目标日期，预计4月，美国FDA将对8款创新药物的批准做出监管决定，本文将对这些疗法进行相关介绍。▲4月美国FDA可能批准的新药（药明康德内容团队制图，点击可见大图）活性成分：Ceftobiprole适应症：金黄色葡萄球菌菌血症、急性细菌性皮肤和皮肤结构感染、社区获得性细菌性肺炎公司名称：Basilea PharmaceuticaCeftobiprole是一款静脉注射的新一代头孢抗生素，对可快速杀死多种革兰氏阳性细菌（如金黄色葡萄球菌，包括耐甲氧西林菌株）和革兰氏阴性菌。它已经在欧洲和中国获批上市。美国FDA已授予其合格传染病产品（QIDP）资格。2023年10月，Basilea Pharmaceutica宣布美国FDA已接受其为ceftobiprole递交的新药申请（NDA），用于治疗三种适应症，包括金黄色葡萄球菌菌血症（SAB）、急性细菌性皮肤和皮肤结构感染（ABSSSI）和社区获得性细菌性肺炎（CABP）。FDA预计在4月3日之前做出审评决定。这一申请得到三项3期临床试验数据的支持，分别为治疗SAB的临床试验ERADICATE、治疗ABSSSI的临床试验TARGET和治疗CABP的一项3期临床试验。Ceftobiprole在试验中与活性对照组相比，均达到非劣效性标准。▲Ceftobiprole分子结构（图片来源：PubChem）活性成分：Anktiva适应症：对卡介苗应答不佳的非肌层浸润性膀胱癌公司名称：ImmunityBioAnktiva是一款白细胞介素-15（IL-15）超级激动剂。IL-15通过影响自然杀伤（NK）细胞和免疫T细胞的发育、维持和功能，在免疫系统中发挥着至关重要的作用。Anktiva由与IL-15受体α/IgG1 Fc融合蛋白结合的IL-15突变体（IL-15N72D）组成。它与βγ T细胞受体结合，直接特异性刺激CD8阳性T细胞和NK细胞，同时避免刺激调节性T细胞（Treg）。与天然、非复合IL-15相比，Anktiva在患者体内具有更优的药代动力学特性，且能在淋巴组织中存在更长时间，表现出增强的抗肿瘤活性。当该疗法与卡介苗（BCG）联用，在治疗对卡介苗应答不佳的非肌层浸润性膀胱癌（NMIBC）的2/3期临床试验中，达到了治疗乳头状瘤亚型患者的主要终点，57%的患者达到12个月的无病生存期（DFS）。2023年10月，FDA接受了ImmunityBio为Anktiva重新递交的BLA，与卡介苗联用，治疗对卡介苗应答不佳的非肌层浸润性膀胱癌。 ▲Anktiva的作用机制（图片来源：ImmunityBio公司官网）活性成分：Pivmecillinam适应症：非复杂性尿路感染公司名称：Utility TherapeuticsPivmecillinam是一种具有独特作用机制的β-内酰胺抗生素，过去40多年里，它已经在多个国家和地区用于治疗尿路感染。在体外和体内研究中，它表现出针对尿路感染中最常见细菌的活性，包括耐药性菌株。今年1月，Utility Therapeutics公司宣布美国FDA已经授予pivmecillinam的新药申请优先审评资格，用于治疗非复杂性尿路感染。该公司的新闻稿指出，这款抗生素表现出95%的临床治愈率，在很多国家和地区被推荐为尿路感染的一线治疗手段。Pivmecillinam和它的静脉注射剂型mecillinam均已获得FDA授予的合格传染病产品资格。NDA申请包括6项支持pivmecillinam疗效的临床研究，12项支持其安全性的研究。▲Pivmecillinam分子结构（图片来源：PubChem）活性成分：Mavorixafor适应症：WHIM综合症公司名称：X4 PharmaceuticalsMavorixafor是一种在研创新的小分子拮抗剂，靶向CXCR4受体。它是专为WHIM综合症和某些类型的慢性中性粒细胞减少症制定的每日一次口服疗法。Mavorixafor已经获得FDA授予突破性疗法认定、快速通道资格、孤儿药资格以及罕见儿科疾病资格。NDA的递交得到了全球性3期关键临床试验4WHIM的支持。这项试验评估每日一次口服mavorixafor在WHIM综合症患者中的疗效和安全性。结果令人鼓舞，4WHIM试验达主要终点与关键次要终点，即药物组患者体内中性粒细胞与淋巴细胞的绝对数量维持在具临床意义阈值之上的时间，明显优于安慰剂组患者（p<0.0001）。美国FDA已授予mavorixafor的NDA优先审评资格，如果获批，mavorixafor将有可能成为WHIM综合征患者的首个疗法。▲CXCR4拮抗剂药理机制（图片来源：X4 Pharmaceuticals官网）活性成分：Tovorafenib适应症：复发性或进展性儿童低度恶性胶质瘤公司名称：Day One BiopharmaceuticalsTovorafenib是一款高度特异性泛RAF激酶抑制剂，它能够抑制携带BRAF融合或BRAF V600突变的肿瘤的生长，并且具有大脑渗透性。它已经获得美国FDA授予的突破性疗法认定和罕见儿科疾病资格，用于治疗携带激活性RAF变异的儿童低度恶性胶质瘤（pLGG）。NDA申请主要是基于包含137位患者的关键性2期试验数据，接受tovorafenib治疗的复发性或进展性pLGG患者总缓解率（ORR）达67%（包含完全缓解[CR]与部分缓解[PR]），以及93%的临床获益率（CBR，即包括CR、PR和疾病稳定[SD]）。分析显示，有17%（n=12）的评估患者达完全缓解，49%（n=34）达部分缓解，26%（n=18）患者为疾病稳定。基于RANO-HGG标准的中位缓解持续时间为16.6个月（95% CI：11.6个月至不可估计）。▲Tovorafenib简介（图片来源：Day One Biopharmaceuticals公司官网）活性成分：mRNA-1345适应症：预防呼吸道合胞病毒（RSV）相关的下呼吸道疾病和急性呼吸疾病公司名称：ModernamRNA-1345是一款编码RSV病毒稳定融合前F糖蛋白的mRNA疫苗，与融合后状态相比，可引起更优的中和抗体反应。它使用与Moderna的新冠疫苗相同的脂质纳米颗粒（LNP）递送，包含优化的蛋白和密码子序列。该疫苗的关键试验达到两个主要疗效终点，针对由两种或两种以上症状定义的RSV相关的下呼吸道疾病（RSV-LRTD）的疫苗有效性为83.7%，针对由三种或三种以上症状定义的RSV-LRTD的疫苗有效性为82.4%。美国FDA已授予mRNA-1345快速通道资格与突破性疗法认定，用以帮助60岁或以上成年人，预防RSV-LRTD和急性呼吸疾病（ARD）。活性成分：Fidanacogene elaparvovec适应症：血友病B公司名称：辉瑞Fidanacogene elaparvovec是一种新型的在研基因疗法，含有生物工程化的AAV衣壳和编码FIX高活性变体的转基因。对于血友病B患者来说，这种基因治疗的目标是使他们能通过一次性治疗产生自体的FIX蛋白，而非像目前的标准治疗那样需要定期静脉输注FIX。上市申请的递交是基于3期BENEGENE-2试验的疗效和安全性数据，此试验共有45名患者入组。分析显示，BENEGENE-2试验达到其主要终点，即与FIX预防性治疗方案相较，患者在经过fidanacogene elaparvovec输注后，其总出血事件的年化出血率（ABR）达到非劣效性与优效性。今年1月，加拿大卫生部（Health Canada）已批准fidanacogene elaparvovec上市（商品名Beqvez），用于治疗18岁或以上中重度至重度血友病B成人患者，这些患者体内不带有靶向AAV血清型Rh74亚型的中和抗体。活性成分：Danicopan适应症：阵发性睡眠性血红蛋白尿症（PNH）公司名称：阿斯利康Danicopan是一款口服补体因子D抑制剂，被设计作为PNH患者的补体C5抑制剂疗法的添加药物。这些患者带有临床上显著的血管外溶血症状。Danicopan可选择性地抑制替代通路中的关键补体因子D，阻断C3转化酶生产而抑制替代通路活性。与C5抑制剂不同的是，danicopan阻止C3b片段在患者血红细胞上的沉积，控制PNH患者红细胞分解与血管外溶血，进而改善患者的治疗效果。NDA的递交主要基于随机双盲关键性3期试验ALPHA的积极结果。试验评估了danicopan作为Ultomiris或Soliris附加疗法，对经历临床显著血管外溶血的PNH患者的疗效和安全性。结果显示，danicopan达到了从基线到第12周血红蛋白变化的主要终点以及所有关键的次要终点，包括避免输血和慢性病治疗功能评估–疲劳（FACIT-Fatigue）评分的变化。今年1月，阿斯利康宣布danicopan已经获得日本厚生劳动省（MHLW）批准（商品名Voydeya），作为标准疗法补体因子C5抑制剂Ultomiris或Soliris的附加疗法，用于那些接受C5抑制剂治疗时发生显著血管外溶血的阵发性睡眠性血红蛋白尿症患者亚群。大家都在看▲欲了解更多前沿技术在生物医药产业中的应用，请长按扫描上方二维码，即可访问“药明直播间”，观看相关话题的直播讨论与精彩回放参考资料：[1] Basilea announces FDA acceptance of New Drug Application for antibiotic ceftobiprole. Retrieved March 29, 2024, from https://www.basilea.com/news#news_1448[2] FDA to review European-approved oral antibiotic for urinary tract infections. Retrieved March 29, 2024, from https://www.cidrap.umn.edu/antimicrobial-stewardship/fda-review-european-approved-oral-antibiotic-urinary-tract-infections免责声明：药明康德内容团队专注介绍全球生物医药健康研究进展。本文仅作信息交流之目的，文中观点不代表药明康德立场，亦不代表药明康德支持或反对文中观点。本文也不是治疗方案推荐。如需获得治疗方案指导，请前往正规医院就诊。版权说明：本文来自药明康德内容团队，欢迎个人转发至朋友圈，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载授权请在「药明康德」微信公众号回复“转载”，获取转载须知。分享，点赞，在看，聚焦全球生物医药健康创新

快速通道临床3期临床结果

100 项与美西林相关的药物交易

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