Molecular Modelling Guided Modulation of Molecular Shape and Charge for Design of Smart Self-Assembled Polymeric Drug Transporters

Nikkhah, Sousa Javan; Thompson, Damien

doi:10.3390/pharmaceutics13020141

Cited by 12 publications

(10 citation statements)

References 211 publications

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“…It is needless to say how helpful having a deep understanding of the affinity contributions of attractive and repulsive interactions and the entropy contribution can be to engineer and tune supramolecular-based therapeutic vehicles. As one of the most effective tools, the multiscale modeling approach holds great promise in predicting the structure and response behavior of materials in various disciplines, including the design of drug carriers. , Visualization of experimental data in a three-dimensional atomic-scale model can assist in explaining phenomena and often raises new questions, thereby improving future research. − However, to study and design effective drug delivery systems using molecular modeling, a broad range of length and time scales needs to be spanned. In this regard, understanding the capabilities of different molecular modeling techniques such as ab initio quantum mechanics (QM), molecular dynamics (MD), Monte Carlo (MC) methods, and mesoscale (MS) methods in the drug delivery systems studies can assist us to select and well-parametrize proper modeling tools (more details of the simulation methods are presented in Table ).…”

Section: Introductionmentioning

confidence: 99%

“…In this regard, understanding the capabilities of different molecular modeling techniques such as ab initio quantum mechanics (QM), molecular dynamics (MD), Monte Carlo (MC) methods, and mesoscale (MS) methods in the drug delivery systems studies can assist us to select and well-parametrize proper modeling tools (more details of the simulation methods are presented in Table ). ,− From all these methods, QM techniques can explain any molecular systems behaviors at the atomistic level by computing the electron distribution but are limited in the system size they can tackle . All noncovalent interactions of various systems at atomic resolution can be monitored using MD simulations. , However, many critical problems in the drug delivery field happen at larger time and length scales far beyond what can be tackled using atomistic MD (force field).…”

Section: Introductionmentioning

confidence: 99%

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Modeling Polyzwitterion-Based Drug Delivery Platforms: A Perspective of the Current State-of-the-Art and Beyond

Nikkhah

Vandichel

2022

ACS Eng. Au

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Drug delivery platforms are anticipated to have biocompatible and bioinert surfaces. PEGylation of drug carriers is the most approved method since it improves water solubility and colloid stability and decreases the drug vehicles’ interactions with blood components. Although this approach extends their biocompatibility, biorecognition mechanisms prevent them from biodistribution and thus efficient drug transfer. Recent studies have shown (poly)zwitterions to be alternatives for PEG with superior biocompatibility. (Poly)zwitterions are super hydrophilic, mainly stimuli-responsive, easy to functionalize and they display an extremely low protein adsorption and long biodistribution time. These unique characteristics make them already promising candidates as drug delivery carriers. Furthermore, since they have highly dense charged groups with opposite signs, (poly)zwitterions are intensely hydrated under physiological conditions. This exceptional hydration potential makes them ideal for the design of therapeutic vehicles with antifouling capability, i.e., preventing undesired sorption of biologics from the human body in the drug delivery vehicle. Therefore, (poly)zwitterionic materials have been broadly applied in stimuli-responsive “intelligent” drug delivery systems as well as tumor-targeting carriers because of their excellent biocompatibility, low cytotoxicity, insignificant immunogenicity, high stability, and long circulation time. To tailor (poly)zwitterionic drug vehicles, an interpretation of the structural and stimuli-responsive behavior of this type of polymer is essential. To this end, a direct study of molecular-level interactions, orientations, configurations, and physicochemical properties of (poly)zwitterions is required, which can be achieved via molecular modeling, which has become an influential tool for discovering new materials and understanding diverse material phenomena. As the essential bridge between science and engineering, molecular simulations enable the fundamental understanding of the encapsulation and release behavior of intelligent drug-loaded (poly)zwitterion nanoparticles and can help us to systematically design their next generations. When combined with experiments, modeling can make quantitative predictions. This perspective article aims to illustrate key recent developments in (poly)zwitterion-based drug delivery systems. We summarize how to use predictive multiscale molecular modeling techniques to successfully boost the development of intelligent multifunctional (poly)zwitterions-based systems.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Modeling Polyzwitterion-Based Drug Delivery Platforms: A Perspective of the Current State-of-the-Art and Beyond

Nikkhah

Vandichel

2022

ACS Eng. Au

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“…We use a dissipative particle dynamics (DPD) coarse-grained molecular model commonly applied in studies of self-assemblies, membranes, and complex fluids. − A detailed discussion of the DPD model equations and parameters can be found elsewhere. , In a coarse-grained molecular model approach, such as DPD, beads represent groups of molecules or atoms, mapping the geometry and momentum of a section of fluid. , In DPD simulations, the particles interact through a soft repulsion potential, which allows the nonbonded particles to overlap. Therefore, two particles of opposite point charge may form an artificial ion-pair.…”

Section: Methodsmentioning

confidence: 99%

Copolyelectrolyte-Based Nanocapsules for Oral Monoclonal Antibody Therapy: A Mesoscale Modeling Survey

Nikkhah

Thompson

2022

Biomacromolecules

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Antibody therapy generally requires parenteral injection to attain the required bioavailability and pharmacokinetics, but improved formulations may slow enzymatic degradation of the antibody in the gastrointestinal tract, permitting the use of noninvasive oral delivery. Rationally designed carrier materials can potentially improve therapeutic activity both by shielding fragile biopharmaceuticals from proteolytic degradation and targeting specific receptors in vivo. One potentially useful class of protein carriers is block copolyelectrolytes, one polyelectrolyte plus one neutral hydrophilic polymer block, that self-assemble into stable micelles, providing a simple and biocompatible nanocapsule separating the protein from the outer medium. Here, we develop and implement an integrated mesoscale model to design molecular structures for block copolyelectrolyte nanocapsules predicted to protect Trastuzumab, an antibody used to treat breast cancer, in the low pH gastrointestinal tract and to selectively release this antibody in the more neutral intestinal environment. The simulations show a tightly packed self-assembled core–shell structure at pH = 3 that is ruptured and dynamically reassembled into a weaker structure at pH = 7. Our model identifies that the designed block copolyelectrolyte characteristics, such as block length ratio, can control the level of drug protection and release in vivo, providing simple design rules for engineering polyelectrolyte-based formulations that may allow oral administration of targeted antibody chemotherapies.

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“…Stimuli-responsive polymers, so-called smart polymers, are the key factor in the latest generation of supramolecular nanocarriers, which are formed through the combination of the two categories. These polymers are able to undergo physicochemical changes or rearrangements due to their response to a specific stimulus, whether that be endogenous, such as to pH and redox variations, hypoxia, and enzymes, or exogenous, such as temperature alterations, light exposure, magnetic fields, and ultrasound, thereby enabling controlled release of active pharmaceutical ingredients (API) at specific sites [32,34,35].…”

Section: Polymeric Nanostructuresmentioning

confidence: 99%

Polymeric Nanostructures Containing Proteins and Peptides for Pharmaceutical Applications

2022

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Over the last three decades, proteins and peptides have attracted great interest as drugs of choice for combating a broad spectrum of diseases, including diabetes mellitus, cancer, and infectious and neurological diseases. However, the delivery of therapeutic proteins to target sites should take into account the obstacles and limitations related to their intrinsic sensitivity to different environmental conditions, fragile tertiary structures, and short half-life. Polymeric nanostructures have emerged as competent vehicles for protein delivery, as they are multifunctional and can be tailored according to their peculiarities. Thus, the enhanced bioavailability and biocompatibility, the adjustable control of physicochemical features, and the colloidal stability of polymer-based nanostructures further enable either the embedding or conjugation of hydrophobic or hydrophilic bioactive molecules, which are some of the features of paramount importance that they possess and which contribute to their selection as vehicles. The present review aims to discuss the prevalent nanostructures composed of block copolymers from the viewpoint of efficient protein hospitality and administration, as well as the up-to-date scientific publications and anticipated applications of polymeric nanovehicles containing proteins and peptides.

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Molecular Modelling Guided Modulation of Molecular Shape and Charge for Design of Smart Self-Assembled Polymeric Drug Transporters

Cited by 12 publications

References 211 publications

Modeling Polyzwitterion-Based Drug Delivery Platforms: A Perspective of the Current State-of-the-Art and Beyond

Modeling Polyzwitterion-Based Drug Delivery Platforms: A Perspective of the Current State-of-the-Art and Beyond

Copolyelectrolyte-Based Nanocapsules for Oral Monoclonal Antibody Therapy: A Mesoscale Modeling Survey

Polymeric Nanostructures Containing Proteins and Peptides for Pharmaceutical Applications

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