TY - JOUR A1 - Güntzel, Paul A1 - Schilling, Klaus A1 - Hanio, Simon A1 - Schlauersbach, Jonas A1 - Schollmayer, Curd A1 - Meinel, Lorenz A1 - Holzgrabe, Ulrike T1 - Bioinspired Ion Pairs Transforming Papaverine into a Protic Ionic Liquid and Salts JF - ACS Omega N2 - Microbial, mammalian, and plant cells produce and contain secondary metabolites, which typically are soluble in water to prevent cell damage by crystallization. The formation of ion pairs, for example, with carboxylic acids or mineral acids, is a natural blueprint to maintain basic metabolites in solution. Here, we aim at showing whether the mostly large carboxylates form soluble protic ionic liquids (PILs) with the basic natural product papaverine resulting in enhanced aqueous solubility. The obtained PILs were characterized by H-1-N-15 HMBC nuclear magnetic resonance (NMR) and in the solid state using X-ray powder diffraction, differential scanning calorimetry, and dissolution measurements. Furthermore, their supramolecular pattern in aqueous solution was studied by means of potentiometric and photometrical solubility, NMR aggregation assay, dynamic light scattering, zeta potential, and viscosity measurements. Thereby, we identified the naturally occurring carboxylic acids, citric acid, malic acid, and tartaric acid, as being appropriate counterions for papaverine and which will facilitate the formation of PILs with their beneficial characteristics, like the improved dissolution rate and enhanced apparent solubility. KW - solubility KW - transport KW - strategy KW - drugs KW - forms KW - acids Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-230265 VL - 5 IS - 30 ER - TY - JOUR A1 - Schlauersbach, Jonas A1 - Hanio, Simon A1 - Lenz, Bettina A1 - Vemulapalli, Sahithya P. B. A1 - Griesinger, Christian A1 - Pöppler, Ann-Christin A1 - Harlacher, Cornelius A1 - Galli, Bruno A1 - Meinel, Lorenz T1 - Leveraging bile solubilization of poorly water-soluble drugs by rational polymer selection JF - Journal of Controlled Release N2 - Poorly water-soluble drugs frequently solubilize into bile colloids and this natural mechanism is key for efficient bioavailability. We tested the impact of pharmaceutical polymers on this solubilization interplay using proton nuclear magnetic resonance spectroscopy, dynamic light scattering, and by assessing the flux across model membranes. Eudragit E, Soluplus, and a therapeutically used model polymer, Colesevelam, impacted the bile-colloidal geometry and molecular interaction. These polymer-induced changes reduced the flux of poorly water-soluble and bile interacting drugs (Perphenazine, Imatinib) but did not impact the flux of bile non-interacting Metoprolol. Non-bile interacting polymers (Kollidon VA 64, HPMC-AS) neither impacted the flux of colloid-interacting nor colloid-non-interacting drugs. These insights into the drug substance/polymer/bile colloid interplay potentially point towards a practical optimization parameter steering formulations to efficient bile-solubilization by rational polymer selection. KW - polymer drug interaction KW - flux KW - bile salt KW - simulated intestinal fluid KW - colloid Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-296957 VL - 330 ET - Accepted Version ER - TY - JOUR A1 - Schlauersbach, Jonas A1 - Hanio, Simon A1 - Raschig, Martina A1 - Lenz, Bettina A1 - Scherf-Cavel, Oliver A1 - Meinel, Lorenz T1 - Bile and excipient interactions directing drug pharmacokinetics in rats JF - European Journal of Pharmaceutics and Biopharmaceutics N2 - Bile solubilization plays a major role in the absorption of poorly water-soluble drugs. Excipients used in oral drug formulations impact bile-colloidal properties and their molecular interactions. Polymer-induced changes of bile colloids, e.g., by Eudragit E, reduced the flux of the bile interacting drug Perphenazine whereas bile non-interacting Metoprolol was not impacted. This study corroborates these in vitro findings in rats. Eudragit E significantly reduced systemic availability of Perphenazine but not Metoprolol compared to the oral administrations without polymer. This study confirms the necessity to carefully select polymers for bile interacting drugs whereas non-bile interacting drugs are more robust in terms of excipient choice for formulation. The perspective of bile interaction may introduce interesting biopharmaceutical leverage for better performing oral formulations of tomorrow. KW - in vitro-in vivo correlation KW - pharmacokinetics KW - bile KW - excipient KW - rat study Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-296969 VL - 178 ET - accepted version ER - TY - JOUR A1 - Spangardt, Christoph A1 - Keßler, Christoph A1 - Dobrzewski, Ramona A1 - Tepler, Antonia A1 - Hanio, Simon A1 - Klaubert, Bernd A1 - Meinel, Lorenz T1 - Leveraging dissolution by autoinjector designs JF - Pharmaceutics N2 - Chemical warfare or terrorism attacks with organophosphates may place intoxicated subjects under immediate life-threatening and psychologically demanding conditions. Antidotes, such as the oxime HI-6, which must be formulated as a powder for reconstitution reflecting the molecule’s light sensitivity and instability in aqueous solutions, dramatically improve recovery—but only if used soon after exposure. Muscle tremors, anxiety, and loss of consciousness after exposure jeopardize proper administration, translating into demanding specifications for the dissolution of HI-6. Reflecting the patients’ catastrophic situation and anticipated desire to react immediately to chemical weapon exposure, the dissolution should be completed within ten seconds. We are developing multi-dose and single-dose autoinjectors to reliably meet these dissolution requirements. The temporal and spatial course of dissolution within the various autoinjector designs was profiled colorimetrically. Based on these colorimetric insights with model dyes, we developed experimental setups integrating online conductometry to push experiments toward the relevant molecule, HI-6. The resulting blueprints for autoinjector designs integrated small-scale rotor systems, boosting dissolution across a wide range of viscosities, and meeting the required dissolution specifications driven by the use of these drug products in extreme situations. KW - autoinjector KW - dissolution KW - oxime KW - response surface KW - nerve agent Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-297271 SN - 1999-4923 VL - 14 IS - 11 ER - TY - THES A1 - Hanio, Simon T1 - The impact of bile on intestinal permeability of drug substances T1 - Der Einfluss der Galle auf die intestinale Permeabilität von Arzneimittelwirkstoffen N2 - Most medicines are taken orally. To enter the systemic circulation, they dissolve in the intestinal fluid, cross the epithelial barrier, and pass through the liver. Intestinal absorption is driven by the unique features of the gastrointestinal tract, including the bile colloids formed in the lumen and the mucus layer covering the intestinal epithelium. Neglecting this multifaceted environment can lead to poor drug development decisions, especially for poorly water-soluble drugs that interact with bile and mucus. However, there is a lack of a rationale nexus of molecular interactions between oral medicines and gastrointestinal components with drug bioavailability. Against this background, this thesis aims to develop biopharmaceutical strategies to optimize the presentation of oral therapeutics to the intestinal epithelial barrier. In Chapter 1, the dynamics of bile colloids upon solubilization of the poorly-water soluble drug Perphenazine was studied. Perphenazine impacted molecular arrangement, structure, binding thermodynamics, and induced a morphological transition from vesicles to worm-like micelles. Despite these dynamics, the bile colloids ensured stable relative amounts of free drug substance. The chapter was published in Langmuir. Chapter 2 examined the impact of pharmaceutical polymeric excipients on bile-mediated drug solubilization. Perphenazine and Imatinib were introduced as model compounds interacting with bile, whereas Metoprolol did not. Some polymers altered the arrangement and geometry of bile colloids, thereby affecting the molecularly soluble amount of those drugs interacting with bile. These insights into the bile-drug-excipient interplay provide a blueprint to optimizing formulations leveraging bile solubilization. The chapter was published in Journal of Controlled Release. Chapter 3 deals with the impact of bile on porcine intestinal mucus. Mucus exposed to bile solution changed transiently, it stiffened, and the overall diffusion rate increased. The bile-induced changes eased the transport of the bile-interacting drug substance Fluphenazine, whereas Metoprolol was unaffected. This dichotomous pattern was linked to bioavailability in rats and generalized based on two previously published data sets. The outcomes point to a bile-mucus interaction relevant to drug delivery. The chapter is submitted. The Appendix provides a guide for biopharmaceutical characterization of drug substances by nuclear magnetic resonance spectroscopy aiming at establishing a predictive algorithm. In summary, this thesis deciphers bile-driven mechanisms shaping intestinal drug absorption. Based on these molecular insights, pharmaceuticals can be developed along a biopharmaceutical optimization, ultimately leading to better oral drugs of tomorrow. N2 - Die meisten Arzneimittel werden oral eingenommen. Um in den Blutkreislauf zu gelangen, liegen sie in der Darmflüssigkeit gelöst vor, überwinden die Epithelbarriere und passieren die Leber. Die intestinale Absorption wird durch die einzigartigen Eigenschaften des Magen-Darm-Trakts, einschließlich der im Lumen gebildeten Gallenkolloide und der Schleimschicht, die das Darmepithel bedeckt, bestimmt. Die Vernachlässigung dieser facettenreichen Umgebung kann zu schlechten Entscheidungen bei der Arzneimittelentwicklung führen, insbesondere bei schlecht wasserlöslich Wirkstoffen, die mit Galle und Schleim interagieren. Es fehlt jedoch eine rationale Verknüpfung der molekularen Wechselwirkungen zwischen oralen Arzneimitteln und gastrointestinalen Komponenten mit der Bioverfügbarkeit von Arzneimitteln. Vor diesem Hintergrund zielt diese Arbeit darauf ab, biopharmazeutische Strategien zur Optimierung der Präsentation von oralen Therapeutika an der intestinalen Epithelbarriere zu entwickeln. In Kapitel 1 wurde die Dynamik von Gallenkolloiden bei der Solubilisierung des schwer wasserlöslichen Wirkstoffes Perphenazin untersucht. Perphenazin beeinflusste die molekulare Anordnung, die Struktur sowie die Bindungsthermodynamik und führte zu einem morphologischen Übergang von Vesikeln hin zu wurmartigen Mizellen. Trotz dieser Dynamik sorgten die Gallenkolloide für stabile relative Mengen an freiem Arzneistoff. Dieses Kapitel wurde in Langmuir veröffentlicht. In Kapitel 2 wurde der Einfluss von pharmazeutischen polymeren Hilfsstoffen auf die Solubilisierung von Wirkstoffen durch Galle untersucht. Perphenazin und Imatinib wurden als Modellverbindungen eingeführt, die mit der Galle interagieren, während Metoprolol dies nicht tat. Einige Polymere veränderten die Anordnung und Geometrie der Gallenkolloide und beeinflussten somit die molekular lösliche Menge von solchen Wirkstoffen, die mit der Galle wechselwirken. Diese Einblicke in das Zusammenspiel von Galle und Arzneistoffen bieten einen Ansatz zur Optimierung von Formulierungen, die die Solubilisierung in der Galle nutzen. Dieses Kapitel wurde in Journal of Controlled Release veröffentlicht. Kapitel 3 befasst sich mit den Auswirkungen von Galle auf den Dünndarmschleim von Schweinen. Schleim, der Gallenlösung ausgesetzt war, veränderte sich vorübergehend, versteifte sich und die Gesamtdiffusionsrate nahm zu. Die durch die Galle hervorgerufenen Veränderungen erleichterten den Transport des mit der Galle interagierenden Wirkstoffs Fluphenazin, während Metoprolol unbeeinflusst blieb. Dieses dichotome Muster konnte mit der Bioverfügbarkeit bei Ratten verknüpft werden und durch zwei zuvor veröffentlichte Datensätze mit insgesamt 50 Verbindungen verallgemeinert werden. Die Ergebnisse deuten auf eine Wechselwirkung zwischen Galle und Schleim hin, die für die Verabreichung von Medikamenten relevant ist. Dieses Kapitel ist eingereicht. Der Anhang bietet einen Leitfaden für die biopharmazeutische Charakterisierung von Arzneimittelsubstanzen durch kernmagnetische Resonanzspektroskopie mit dem Ziel des Aufstellens von prädiktiven Algorithmen. Zusammenfassend entschlüsselt diese Arbeit die von der Galle gesteuerten Mechanismen, die die Aufnahme von Arzneimitteln im Darm beeinflussen. Auf der Grundlage dieser molekularen Erkenntnisse können Arzneimittel entlang einer biopharmazeutischen Optimierung entwickelt werden, was letztendlich zu besseren oralen Arzneimitteln führt. KW - Solubilisation KW - Galle KW - Bioverfügbarkeit KW - Pharmazeutischer Hilfsstoff KW - drug delivery KW - absorption KW - intestinal permeability KW - poor water-soluble drugs KW - intestinal mucus KW - pig KW - drug formulation KW - molecular biopharmaceutics KW - mucin KW - Schleim KW - Bile KW - Mucus Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-348906 ER -