Synthesis, characterization and biological activity of Schiff bases based on chitosan and arylpyrazole moiety
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*Manuscript Click here to view linked References Page 6 of 31 Accepted Manuscript 2 1. Introduction Chitosan ( β -(1–4)-linked-d-glucosamine) is obtained by the deacetylation of chitin ( β -(1–4)-linked N-acetyl-d-glucosamine), one of the most abundant natural polysaccharide in nature [1, 2]. Its structure is basically constituted of D-glucosamine units, with contents of N-acetyl-D-glucosamine in the range of 0–50% [3]. This polysaccharide displays interesting properties, such as abundant resources, nontoxicity, biodegradability, biocompatibility, and antibacterial properties. Therefore, it has prospective applications in many fields such as agriculture, pharmaceuticals, cosmetics, food industries, environmental protection, and biotechnology [4-10]. Antibacterial activity is one of the most important bioactivities of chitosan. It has been shown to be an effective agent against an array of common bacteria (Gram-positive as well as Gram-negative) and fungi [11]. Moreover, chitosan has several advantages over other types of antimicrobial agents because it possesses a higher antibacterial activity, a broader spectrum of activity, a higher killing rate, and a lower toxicity toward mammalian cells [12]. The reactive amino and hydroxyl groups of chitosan can be used to chemically alter its properties under mild reaction conditions [13 -16 ]. The derivation is intended to improve its processability, solubility, antimicrobial activity and its ability to interact with other substances [ 17- 21]. One of the most important modifications is related to Schiff bases, which are formed from the condensation of amino groups on the chitosan with the added aldehyde or ketone [22-26]. These materials are economically feasible and widely used in the field of biocides [21, 27] and in coordination chemistry [28- 31]. For instance, such Schiff bases can be chelated with various metal ions and be used as heterogeneous catalysts [32-34]. On the other hand, pyrazoles are of interest as potent bioactive molecules in pharmaceutical development and possess a wide range of biological activities [35, 36]. Besides being biologically active, they are also used as useful synthons in organic synthesis [37]. Based on the above consideration, the modification of chitosan with pyrazoles as substituent may improve some of the physical properties and antimicrobial activity of chitosan. Therefore, the aim of the present study is to develop new chitosan Schiff bases with arylpyrazole moiety. These compounds will be characterized by various methods, such as FT-IR, XRD, elemental and thermal analyses. The antimicrobial assays of the prepared chitosan derivatives against Streptococcus pneumoniae (S. pneumonia, RCMB 010010) and Bacillis subtilis (B. subtilis, RCMB 010067) as Gram positive bacteria, and against Escherichia coli (E. coli, RCMB 010052) as Gram negative bacteria and against Aspergillus fumigatus (A. fumigatus, RCMB 02568), Geotricum candidum (G. |
