Trimethylammonium-Based Polymethacrylate Ionic Liquids with Tunable Hydrophilicity and Charge Distribution as Carriers of Salicylate Anions

Bielas, Rafał; Mielańczyk, Anna; Siewniak, Agnieszka; Neugebauer, Dorota

doi:10.1021/acssuschemeng.6b00690

Cited by 25 publications

(22 citation statements)

References 36 publications

(55 reference statements)

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“…This molecule supports biological functions [ 34 , 37 , 38 ] as a precursor of acetylcholine [ 39 ]. The presence of an ionic group in the cholinium unit gives the opportunity for the ion exchange reaction, which in the case of polymerized ionic liquids can be advantageous for incorporation of pharmaceutical ions, i.e., sulfacetamid, salicylate [ 40 , 41 , 42 ]. There are also reports of other types of PILs, based on imidazolium and pyridinium transporting naproxen anions [ 43 ] or guanidinium with ampicillin anions [ 44 ].…”

Section: Introductionmentioning

confidence: 99%

Synthesis and Characterization of Ionic Graft Copolymers: Introduction and In Vitro Release of Antibacterial Drug by Anion Exchange

Niesyto

Neugebauer

2020

Polymers

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Amphiphilic graft copolymers based on [2-(methacryloyloxy)ethyl]trimethyl- ammonium chloride (TMAMA) were obtained for the delivery of pharmaceutical ionic drugs, such as p-aminosalicylate (PAS) and clavunate (CLV) anions. The side chains were attached by grafting from a multifunctional macroinitiator via atom transfer radical polymerization (ATRP) to get polymers with different grafting degrees and ionic content. The self-assembling ability, confirmed by determining the critical micelle concentration (CMC) through interfacial tension (IFT) with the use of goniometry, was reduced after ion exchange (CMC twice higher than for chloride anions contained copolymers 0.005–0.026 mg/mL). Similarly, the hydrophilicity level (adjusted by the content of ionic fraction) evaluated by the water contact angle (WCA) of the polymer film surfaces was decreased with the increase of trimethylammonium units (68°–44°) and after introduction of pharmaceutical anions. The exchange of Cl− onto PAS− and CLV− in the polymer matrix was yielded at 31%–64% and 79%–100%, respectively. The exchange onto phosphate anions to release the drug was carried out (PAS: 20%–42%, 3.1–8.8 μg/mL; CLV: 25%–73%, 11–31 μg/mL from 1 mg of drug conjugates). Because of the bacteriostatic activity of PAS and the support of the action of the antibiotics by CLV, the designed water-soluble systems could be alternatives for the treatment of bacterial infections, including pneumonia and tuberculosis.

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Section: Introductionmentioning

confidence: 99%

Synthesis and Characterization of Ionic Graft Copolymers: Introduction and In Vitro Release of Antibacterial Drug by Anion Exchange

Niesyto

Neugebauer

2020

Polymers

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“…They gained great interest in material science because of macromolecular architectures, which can be tailored by combining both properties of cations and anions [38]. In our recent studies on the amphiphilic graft copolymers, the monomeric ionic liquids, i.e., commercially available (2-(methacryloyloxy)ethyl)-trimethylammonium chloride (ChMACl known as choline methacrylate) and containing pharmaceutical salicylate anion (ChMASal, [39,40]), were grafted from the standard multifunctional ATRP macroinitiators, i.e., poly(methyl methacrylate- co -(2-(2-bromoisobutyryloxy)ethyl methacrylate))) (poly(MMA- co -BIEM: MI) [41,42] with various contents of bromoester initiating groups, 25–75% (GPIL1 series and GPIL2, Figure 1c, Table 1). The side chains resulted in the use of methyl methacrylate (MMA) as the comonomer.…”

Section: Non-linear Polymers Containing Ionic Groups In Drug Deliverymentioning

confidence: 99%

“…For comparison, the analogous linear poly(ionic liquid)s (LPIL1–2) were synthesized using standard ATRP initiator. i.e., ethyl α-bromoisobutyrate (EBiB) [39,40]. The LPIL systems, both chloride (LPIL2.1) and salicylate (LPIL1.1–1.2) ones in relation to analogical GPIL, exhibited higher drug loading content (DLC LPIL > DLC GPIL ), but this difference was significantly higher for salicylate systems, whereas the opposite DLC dependency was indicated for IMC encapsulation [44].…”

Section: Non-linear Polymers Containing Ionic Groups In Drug Deliverymentioning

confidence: 99%

Ionic Polymethacrylate Based Delivery Systems: Effect of Carrier Topology and Drug Loading

et al. 2019

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The presented drug delivery polymeric systems (DDS), i.e., conjugates and self-assemblies, based on grafted and star-shaped polymethacrylates have been studied for the last few years in our group. This minireview is focused on the relationship of polymer structure to drug conjugation/entrapment efficiency and release capability. Both graft and linear polymers containing trimethylammonium groups showed the ability to release the pharmaceutical anions by ionic exchange, but in aqueous solution they were also self-assembled into nanoparticles with encapsulated nonionic drugs. Star-shaped polymers functionalized with ionizable amine/carboxylic groups were investigated for drug conjugation via ketimine/amide linkers. However, only the conjugates of polybases were water-soluble, giving opportunity for release studies, whereas the self-assembling polyacidic stars were encapsulated with the model drugs. Depending on the type of drug loading in the polymer matrix, their release rates were ordered as follows: Physical ≥ ionic > covalent. The studies indicated that the well-defined ionic polymethacrylates, including poly(ionic liquid)s, are advantageous for designing macromolecular carriers due to the variety of structural parameters, which are efficient for tuning of drug loading and release behavior in respect to the specific drug interactions.

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“…There remains considerable research into the design of supramolecular gelation layers than can encapsulate salicylates—and MS, in particular, with the aim of enhancing the biocompatibility of the host matrix and enabling more controllable release of the therapeutic agent [ 62 , 63 , 64 ]. While there are numerous formulations available, it is important to note that very few have been approved by the FDA for the temporary relief of pain relative to the many conditions associated with chronic pain, as indicated in Table 2 .…”

Section: Technological Solutionsmentioning

confidence: 99%

Salicylate Poisoning Potential of Topical Pain Relief Agents: From Age Old Remedies to Engineered Smart Patches

et al. 2017

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The pain relief capabilities of methyl salicylate are well established and a multitude of over-the-counter products populate pharmacy shelves. Over-application of the topical preparation containing the drug, or its accidental ingestion, invariably result in salicylate poisoning and in severe cases can be fatal. The drug has been a regular feature of the US National Poison Database Survey over the past decade and continues to pose a risk to children and adults alike. The aim of the review has been to cast a spotlight on the drug and assess why its use remains problematic, how technology could offer more efficacious delivery regimes, and minimise the possibility of accidental or intentional misuse.

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Trimethylammonium-Based Polymethacrylate Ionic Liquids with Tunable Hydrophilicity and Charge Distribution as Carriers of Salicylate Anions

Cited by 25 publications

References 36 publications

Synthesis and Characterization of Ionic Graft Copolymers: Introduction and In Vitro Release of Antibacterial Drug by Anion Exchange

Synthesis and Characterization of Ionic Graft Copolymers: Introduction and In Vitro Release of Antibacterial Drug by Anion Exchange

Ionic Polymethacrylate Based Delivery Systems: Effect of Carrier Topology and Drug Loading

Salicylate Poisoning Potential of Topical Pain Relief Agents: From Age Old Remedies to Engineered Smart Patches

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