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Transdermal drug delivery system of lidocaine hydrochloride based on dissolving gelatin/sodium carboxymethylcellulose microneedles 基于溶解明胶/羧甲基纤维素钠微针的盐酸利多卡因透皮给药系统
Pub Date : 2023-04-03 DOI: 10.1186/s41120-023-00074-9
Shabnam Bahmani, R. Khajavi, M. Ehsani, M. Rahimi, M. Kalaee
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引用次数: 2
CMC development of [14C]-labeled sotorasib for the conduct of microtracer human ADME study [14C]标记sotorasib的CMC开发用于微示踪人ADME研究
Pub Date : 2023-03-20 DOI: 10.1186/s41120-023-00075-8
Sonika Sharma, Prashant Agarwal, A. T. Parsons, J. Huckle, T. Correll
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引用次数: 0
Development of human-machine language interfaces for the visual analysis of complex biologics and RNA modalities and associated experimental data 开发人机语言界面,用于复杂生物制剂和RNA模式以及相关实验数据的可视化分析
Pub Date : 2023-03-01 DOI: 10.1186/s41120-023-00073-w
R. Kunz, Atipat Rojnuckarin, C. Schmidt, L. Miranda
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引用次数: 1
Simple and rapid method for analysis of urinary vancomycin using solid phase extraction and fluorescence spectroscopy 固相萃取-荧光光谱法分析尿中万古霉素的简便快速方法
Pub Date : 2023-02-06 DOI: 10.1186/s41120-023-00071-y
Yuki Oshima, Mizuki Hori, Miyu Matsumoto, Masaru Kato
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引用次数: 0
Incorporating random effects in biopharmaceutical control strategies 将随机效应纳入生物制药控制策略
Pub Date : 2023-02-01 DOI: 10.1186/s41120-022-00070-5
Thomas Oberleitner, T. Zahel, M. Kunzelmann, Judith Thoma, C. Herwig
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引用次数: 2
Research on Pickering emulsification technology based on the concept of “combination of medicine and adjuvant” to improve the pH stability of volatile oil in solid preparations—taking Lingzhu Pulvis as an Example 基于“药与佐剂结合”理念的Pickering乳化技术提高固体制剂中挥发油pH稳定性的研究——以灵珠蒲为例
Pub Date : 2023-01-10 DOI: 10.1186/s41120-022-00068-z
Lei Peng, Mei Wang, Xiao-Fei Zhang, Dongyan Guo, Bing-tao Zhai, Junbo Zou, Yajun Shi
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引用次数: 1
Structured content and data management-enhancing acceleration in drug development through efficiency in data exchange. 结构化内容和数据管理通过数据交换的效率提高了药物开发的速度。
Pub Date : 2023-01-01 Epub Date: 2023-05-08 DOI: 10.1186/s41120-023-00077-6
Jill Beierle, Marquerita Algorri, Marisol Cortés, Nina S Cauchon, Andrew Lennard, J Paul Kirwan, Shirley Oghamian, Michael J Abernathy

Innovation in pharmaceutical therapeutics is critical for the treatment of serious diseases with unmet medical need. To accelerate the approval of these innovative treatments, regulatory agencies throughout the world are increasingly adopting the use of expedited pathways and collaborative regulatory reviews. These pathways are primarily driven by promising clinical results but become challenging for Chemistry, Manufacturing, and Controls (CMC) information in regulatory submissions. Condensed and shifting timelines present constraints that require new approaches to the management of regulatory filings. This article emphasizes technological advances that have the potential to tackle the underlying inefficiencies in the regulatory filing eco-system. Structured content and data management (SCDM) is highlighted as a foundation for technologies that can ease the burden on both sponsors and regulators by streamlining data usage in regulatory submissions. Re-mapping of information technology infrastructure will improve the usability of data by moving away from document-based filings towards electronic data libraries. Although the inefficiencies of the current regulatory filing eco-system are more evident for products that are filed using expedited pathways, it is envisioned that the more widespread adoption of SCDM, across standard filing and review processes, will improve overall efficiency and speed in the compilation and review of regulatory submissions.

药物治疗的创新对于治疗医疗需求未得到满足的严重疾病至关重要。为了加快批准这些创新治疗方法,世界各地的监管机构越来越多地采用快速途径和合作监管审查。这些途径主要是由有希望的临床结果驱动的,但对监管提交的化学、制造和控制(CMC)信息具有挑战性。紧凑和不断变化的时间表带来了限制,需要对监管文件的管理采取新的方法。这篇文章强调了技术进步有可能解决监管备案生态系统中潜在的低效问题。结构化内容和数据管理(SCDM)被强调为技术的基础,这些技术可以通过简化监管提交中的数据使用来减轻赞助商和监管机构的负担。信息技术基础设施的重新规划将从基于文件的归档转向电子数据库,从而提高数据的可用性。尽管目前监管备案生态系统的低效性在使用快速途径备案的产品中更为明显,但可以预见,在标准备案和审查过程中更广泛地采用SCDM,将提高监管提交文件的编制和审查的整体效率和速度。
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引用次数: 1
Extraction of niclosamide from commercial approved tablets into aqueous buffered solution creates potentially approvable oral and nasal sprays against COVID-19 and other respiratory infections. 从商业批准的片剂中提取氯硝沙胺到水缓冲溶液中,可产生潜在批准的针对COVID-19和其他呼吸道感染的口服和鼻喷雾剂。
Pub Date : 2023-01-01 DOI: 10.1186/s41120-023-00072-x
David Needham

Motivation: The low solubility, weak acid drug, niclosamide is a host cell modulator with broad-spectrum anti-viral cell-activity against many viruses, including stopping the SARS-CoV-2 virus from infecting cells in cell culture. As a result, a simple universal nasal spray preventative was proposed and investigated in earlier work regarding the dissolution of niclosamide into simple buffers. However, starting with pharmaceutical grade, niclosamide represents a new 505(b)(2) application. The motivation for this second paper in the series was therefore to explore if and to what extent niclosamide could be extracted from commercially available and regulatory-approved niclosamide oral tablets that could serve as a preventative nasal spray and an early treatment oral/throat spray, with possibly more expeditious testing and regulatory approval.

Experimental: Measurements of supernatant niclosamide concentrations were made by calibrated UV-Vis for the dissolution of niclosamide from commercially available Yomesan crushed into a powder for dissolution into Tris Buffer (TB) solutions. Parameters tested were as follows: time (0-2 days), concentration (300 µM to -1 mM), pH (7.41 to 9.35), and anhydrous/hydrated state. Optical microscopy was used to view the morphologies of the initial crushed powder, and the dissolving and equilibrating undissolved excess particles to detect morphologic changes that might occur.

Results: Concentration dependence: Niclosamide was readily extracted from powdered Yomesan at pH 9.34 TB at starting Yomesan niclosamide equivalents concentrations of 300 µM, 600 µM, and 1 mM. Peak dissolved niclosamide supernatant concentrations of 264 µM, 216 µM, and 172 µM were achieved in 1 h, 1 h, and 3 h respectively. These peaks though were followed by a reduction in supernatant concentration to an average of 112.3 µM ± 28.4 µM after overnight stir on day 2. pH dependence: For nominal pHs of 7.41, 8.35, 8.85, and 9.35, peak niclosamide concentrations were 4 µM, 22.4 µM, 96.2 µM, and 215.8 µM, respectively. Similarly, the day 2 values all reduced to 3 µM, 12.9 µM, 35.1 µM, and 112.3 µM. A heat-treatment to 200 °C dehydrated the niclosamide and showed a high 3 h concentration (262 µM) and the least day-2 reduction (to 229 µM). This indicated that the presence, or formation during exposure to buffer, of lower solubility polymorphs was responsible for the reductions in total solubilities. These morphologic changes were confirmed by optical microscopy that showed initially featureless particulate-aggregates of niclosamide could grow multiple needle-shaped crystals and form needle masses, especially in the presence of Tris-buffered sodium chloride, where new red needles were rapidly made. Scale up: A scaled-up 1 L solution of niclosamide was made achieving 165 µM supernatant niclosamide in 3 h by dissolution of just one fifth (100 mg niclosamide) of a Yomesan tab

动机:低溶解度、弱酸性药物,氯硝沙胺是一种宿主细胞调节剂,对多种病毒具有广谱抗病毒细胞活性,包括在细胞培养中阻止SARS-CoV-2病毒感染细胞。因此,提出了一种简单的通用鼻喷雾剂,并在早期的工作中研究了氯硝沙胺在简单缓冲液中的溶解。然而,从药物级开始,氯硝柳胺代表了一个新的505(b)(2)申请。因此,该系列第二篇论文的动机是探索是否以及在多大程度上可以从市售和监管部门批准的氯硝柳胺口服片剂中提取氯硝柳胺,这种片剂可以作为预防性鼻喷雾剂和早期治疗口服/咽喉喷雾剂,可能会更快地进行测试和监管部门的批准。实验:用标定的UV-Vis测定上清硝柳胺的浓度,以测定市售的Yomesan粉碎成粉末溶解到Tris缓冲液(TB)溶液中的硝柳胺的溶出度。测试参数如下:时间(0-2天)、浓度(300µM ~ -1 mM)、pH(7.41 ~ 9.35)、无水/水合状态。利用光学显微镜观察粉碎后的初始粉末的形态,以及溶解和平衡未溶解的多余颗粒,以检测可能发生的形态变化。结果:浓度依赖性:在pH为9.34 TB的条件下,Yomesan硝氯胺起始浓度为300µM、600µM和1 mM时,Yomesan硝氯胺很容易从粉末状的Yomesan中提取。在1 h、1 h和3 h时,溶解的硝氯胺上清的峰值浓度分别为264µM、216µM和172µM。这些峰值之后,在第2天过夜后,上清液浓度降低到平均112.3µM±28.4µM。pH依赖性:当pH值为7.41、8.35、8.85和9.35时,氯硝柳胺的峰值浓度分别为4µM、22.4µM、96.2µM和215.8µM。同样,第2天的数值均降至3µM、12.9µM、35.1µM和112.3µM。热处理至200°C使氯硝柳胺脱水,3 h浓度高(262µM),第2天还原最小(229µM)。这表明,在暴露于缓冲液期间,溶解度较低的多晶的存在或形成是导致总溶解度降低的原因。光学显微镜证实了这些形态变化,显示最初无特征的氯硝柳胺颗粒聚集体可以生长出多个针状晶体并形成针状团块,特别是在tris缓冲氯化钠存在的情况下,新的红色针状物质迅速形成。按比例放大:1升奈洛沙胺溶液在3小时内溶出约美散片的五分之一(100mg奈洛沙胺),得到165µM奈洛沙胺上清。结论:这些综合结果为如何利用市售和批准的氯硝柳胺片以简单的溶出工艺制备氯硝柳胺水溶液提供了指导。如图所示,一个4片包装的Yomesan可以很容易地制成165升20µM的氯硝柳胺溶液,相当于16,500瓶10毫升的瓶子。仅60包Yomesan就可生产100万瓶,可提供1亿次单次喷雾剂量,作为全球通用的预防性鼻用和早期治疗口服/咽喉喷雾剂分发,以减轻许多呼吸道感染。图解摘要:由美散碎片料提取的氯硝柳胺在Tris缓冲液(瓶中为黄绿色)和Tris缓冲盐水(瓶中为橙红色)中的pH依赖性。初始无水溶解浓度可通过隔夜搅拌降低为可能的一水硝柳胺;如果在TBSS中形成从原始颗粒生长出来的新的氯胺钠针状晶体,则更低。补充信息:在线版本包含补充资料,下载地址:10.1186/s41120-023-00072-x。
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引用次数: 0
Customer-centric product presentations for monoclonal antibodies. 以客户为中心的单克隆抗体产品介绍。
Pub Date : 2023-01-01 Epub Date: 2023-01-23 DOI: 10.1186/s41120-022-00069-y
Beate Bittner

Delivering customer-centric product presentations for biotherapeutics, such as monoclonal antibodies (mAbs), represents a long-standing and paramount area of engagement for pharmaceutical scientists. Activities include improving experience with the dosing procedure, reducing drug administration-related expenditures, and ultimately shifting parenteral treatments outside of a controlled healthcare institutional setting. In times of increasingly cost-constrained markets and reinforced with the coronavirus pandemic, this discipline of "Product Optimization" in healthcare has gained momentum and changed from a nice-to-have into a must. This review summarizes latest trends in the healthcare ecosystem that inform key strategies for developing customer-centric products, including the availability of a wider array of sustainable drug delivery options and treatment management plans that support dosing in a flexible care setting. Three disease area archetypes with varying degree of implementation of customer-centric concepts are introduced to highlight relevant market differences and similarities. Namely, rheumatoid arthritis and inflammatory bowel disease, multiple sclerosis, and oncology have been chosen due to differences in the availability of subcutaneously dosed and ready-to-use self-administration products for mAb medicines and their follow-on biologics. Different launch scenarios are described from a manufacturer's perspective highlighting the necessity of platform approaches. To unfold the full potential of customer-centric care, value-based healthcare provider reimbursement schemes that incentivize the efficiency of care need to be broadly implemented.

为单克隆抗体(mAbs)等生物治疗药物提供以客户为中心的产品演示,是制药科学家长期参与的一个重要领域。其活动包括改善给药过程的体验、减少给药相关支出,以及最终将肠外治疗转移到受控医疗机构环境之外。在成本日益受限的市场和冠状病毒大流行的背景下,医疗保健领域的 "产品优化 "学科已获得了强劲的发展势头,并从 "不错 "变成了 "必须"。本综述总结了医疗保健生态系统的最新趋势,这些趋势为开发以客户为中心的产品提供了关键策略,包括提供更广泛的可持续给药选择和治疗管理计划,以支持在灵活的护理环境中给药。本文介绍了以客户为中心理念实施程度不同的三个疾病领域原型,以突出相关市场的异同。之所以选择类风湿性关节炎和炎症性肠病、多发性硬化症和肿瘤学,是因为这三个疾病的 mAb 药物及其后续生物制剂在皮下给药和即用型自助给药产品的可用性方面存在差异。从制造商的角度描述了不同的上市方案,强调了平台方法的必要性。为了充分发挥以客户为中心的医疗服务的潜力,需要广泛实施以价值为基础的医疗服务提供者报销计划,以激励医疗服务的效率。
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引用次数: 0
Verification of nanoparticle formation, skin permeation, and apoptosis using nobiletin as a methoxyflavonoid derivative 验证纳米颗粒的形成,皮肤渗透和细胞凋亡使用诺毕尔素作为甲氧基类黄酮衍生物
Pub Date : 2022-11-28 DOI: 10.1186/s41120-022-00065-2
Y. Inoue, Moe Ishizawa, S. Itakura, T. Tanikawa, H. Todo
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引用次数: 0
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AAPS Open
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