ABSTRACT
The implementation of Molecularly Imprinted Polymers (MIPs) into sensing systems has been demonstrated abundantly over the past few decades. In this article, a novel application for an MIP-based thermal sensing platform is introduced by using the sensor to characterize the drug release kinetics of a nanoporous silver-organic framework. This Ag nanoporous matrix was loaded with acetylsalicylic acid (aspirin) which was used as a model drug compound in this study. The drug elution properties were studied by placing the nanoporous matrix in phosphate buffered saline solution for two days and measuring the drug concentration at regular time intervals. To this extent, an acrylamide-based MIP was synthesized that was able to detect aspirin in a specific and selective manner. Rebinding of the template to the MIP was analyzed using a thermal sensor platform. The results illustrate that the addition of aspirin into the sensing chamber leads to a concentration-dependent increase in the phase shift of a thermal wave that propagates through the MIP-coated sensor chip. After constructing a dose-response curve, this system was used to study the drug release kinetics of the nanoporous matrix, clearly demonstrating that the metalorganic framework releases the drug steadily over the course of the first hour, after which the concentration reaches a plateau. These findings were further confirmed by UVâ»Visible spectroscopy, illustrating a similar time-dependent release in the same concentration range, which demonstrates that the MIP-based platform can indeed be used as a low-cost straightforward tool to assess the efficacy of drug delivery systems in a lab environment.
ABSTRACT
A general method for the synthesis of cage-carbon-functionalized cyclopentadienyl iron and cyclopentadienyl ruthenium tricarbadecaboranyl complexes has been developed that employs palladium-catalyzed Sonogashira, Heck, and Stille cross-coupling reactions directed at a cage-carbon haloaryl substituent. The key Li(+)[6-(p-XC(6)H(4))-nido-5,6,9-C(3)B(7)H(9)(-)] (X = I (1), Br (2), Cl (3)) haloaryl-tricarbadecaboranyl anionic ligands were synthesized in high yields via the reaction of the arachno-4,6-C(2)B(7)H(12)(-) anion with the corresponding p-halobenzonitriles (p-XC(6)H(4)-CN). The reactions of the salts 1-3 with (η(5)-C(5)H(5))Fe(CO)(2)I and (η(5)-C(5)H(5))Ru(CH(3)CN)(3)PF(6) were then used to produce the haloaryl complexes 1-(η(5)-C(5)H(5))-2-(p-XC(6)H(4))-closo-1,2,3,4-MC(3)B(7)H(9) (M = Fe, X = I (4), Br (5), Cl (6) and M = Ru, X = I (7), Br (8), Cl (9)). The sonication-promoted Sonogashira coupling reactions of 4 with terminal alkynes catalyzed by Pd(dppf)(2)Cl(2)/CuI yielded the alkynyl-linked derivatives 1-(η(5)-C(5)H(5))-2-p-RC(6)H(4)-closo-1,2,3,4-FeC(3)B(7)H(9) (R = (PhC≡C)- (10), (CH(3)CH(2)C(O)OCH(2)C≡C)- (11), ((η(5)-C(5)H(5))Fe(η(5)-C(5)H(4)C≡C))- (12)). Heck reactions of 4 with terminal alkenes catalyzed by Pd(OAc)(2) yielded the alkene-functionalized products 1-(η(5)-C(5)H(5))-2-p-RC(6)H(4)-closo-1,2,3,4-FeC(3)B(7)H(9) (R = (PhCH(2)CHâCH)- (13), (CH(3)(CH(2))(2)CHâCH)- (14)), while the Stille cross-coupling reactions of 4 with organotin compounds catalyzed by Pd(PPh(3))(2)Cl(2) afforded the complexes 1-(η(5)-C(5)H(5))-2-p-RC(6)H(4)-closo-1,2,3,4-FeC(3)B(7)H(9) (R = Ph- (15), (CH(2)âCH)- (16), (CH(2)âCHCH(2))- (17)). These reactions thus provide facile and systematic access to a wide variety of new types of functionalized metallatricarbadecaboranyl complexes with substituents needed for potential metallocene-like biomedical and/or optoelectronic applications.