Alfei Silvana, Milanese Marco, Brullo Chiara, Valenti Giulia Elda, Domenicotti Cinzia, Russo Eleonora, Marengo Barbara
Section of Chemistry and Pharmaceutical and Food Technologies, Department of Pharmacy, University of Genoa, Viale Cembrano, 4, 16148 Genoa, Italy.
Section of Medicinal Chemistry and Cosmetic Product, Department of Pharmacy (DIFAR), University of Genoa, Viale Benedetto XV, 3, 16132 Genoa, Italy.
Pharmaceutics. 2023 Oct 4;15(10):2425. doi: 10.3390/pharmaceutics15102425.
Aiming at developing a dermal formulation against melanoma, the synthesized imidazo-pyrazoles 2-phenyl-2,3-dihydro-1H-imidazo[1,2-b]pyrazole-7-carboxylic acid (3-methoxy-4-phenoxy-benzylidene)-hydrazide () and 2-phenyl-2,3-dihydro-1H-imidazo[1,2-b]pyrazole-7-carboxylic acid (4-benzyloxy-3-methoxy-benzylidene)-hydrazide () were screened on patient-isolated melanoma cells (MEOV NT) and on Vemurafenib (PLX4032)-resistant (MEOV PLX-R) ones. Since on MEOV PLX-R cells was 1.4-fold more effective than PLX, a hydrogel formulation containing (R4HG-4I) was prepared in parallel with an empty R4-based hydrogel (R4HG) using a synthesized antibacterial resin (R4) as gelling agent. Thanks to its high hydrophilicity, porosity (85%), and excellent swelling capability (552%), R4 allowed to achieve R4HG and R4HG-4I with high equilibrium degree of swelling (EDS) and equilibrium water content (EWC). Chemometric-assisted ATR-FTIR analyses confirmed the chemical structure of swollen and fully dried (R4HG-D and R4HG-4I-D) hydrogels. The morphology of R4HG-D and R4HG-4I-D was examined by optical microscopy and SEM, while UV-vis analyses were carried out to obtain the drug loading (DL%) and the encapsulation efficiency (EE%) of R4HG-4I. Potentiometric titrations were performed to determine the equivalents of NH in both R4HG and R4HG-4I. The swelling and water release profiles of both materials and related kinetics were assessed by equilibrium swelling rate and water loss studies, respectively, while their biodegradability over time was assessed by in vitro degradation experiments determining their mass loss. Rheological experiments established that both R4HG and R4HG-4I are shear-thinning Bingham pseudoplastic fluids with low yield stress, thus assuring easy spreadability in a future topical application. Release studies evidenced a sustained and quantitative release of governed mainly by diffusion. Upon favorable results from further experiments in a more realistic 3D model of melanoma, R4HG-4I could represent a starting point to develop new topical therapeutic options to adjuvate the treatments of melanoma cells also when resistant to currently available drugs.
为了开发一种针对黑色素瘤的皮肤制剂,对合成的咪唑并吡唑类化合物2-苯基-2,3-二氢-1H-咪唑并[1,2-b]吡唑-7-羧酸(3-甲氧基-4-苯氧基-亚苄基)-酰肼()和2-苯基-2,3-二氢-1H-咪唑并[1,2-b]吡唑-7-羧酸(4-苄氧基-3-甲氧基-亚苄基)-酰肼()在患者分离的黑色素瘤细胞(MEOV NT)和对维莫非尼(PLX4032)耐药的(MEOV PLX-R)细胞上进行了筛选。由于在MEOV PLX-R细胞上的效果比PLX高1.4倍,因此使用合成抗菌树脂(R4)作为胶凝剂,与空的基于R4的水凝胶(R4HG)并行制备了含有(R4HG-4I)的水凝胶制剂。由于R4具有高亲水性、孔隙率(85%)和优异的溶胀能力(552%),使得能够制备出具有高平衡溶胀度(EDS)和平衡含水量(EWC)的R4HG和R4HG-4I。化学计量学辅助的ATR-FTIR分析证实了溶胀和完全干燥的(R4HG-D和R4HG-4I-D)水凝胶的化学结构。通过光学显微镜和扫描电子显微镜检查了R4HG-D和R4HG-4I-D的形态,同时进行了紫外-可见分析以获得R4HG-4I的载药量(DL%)和包封率(EE%)。进行电位滴定以确定R4HG和R4HG-4I中NH的当量。分别通过平衡溶胀率和水分损失研究评估了两种材料的溶胀和水释放曲线及其相关动力学,同时通过体外降解实验测定其质量损失来评估它们随时间的生物降解性。流变学实验表明,R4HG和R4HG-4I均为具有低屈服应力的剪切变稀宾汉假塑性流体,从而确保在未来局部应用中易于铺展。释放研究表明,的释放持续且定量,主要受扩散控制。在更真实的黑色素瘤3D模型中进行的进一步实验取得良好结果后,R4HG-4I可能成为开发新的局部治疗方案的起点,以辅助黑色素瘤细胞的治疗,即使在对现有药物耐药时也是如此。
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