Liposomal vaccine formulations as prophylactic agents: design considerations for modern vaccines
participate in pathogen opsonization. However, most
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participate in pathogen opsonization. However, most PRRs are transmembrane (like C-type lectin and Toll- like receptors; CLRs and TLRs, respectively) or cytosolic (retinoic acid-inducible gene I and nucleotide-binding domain and leucine-rich repeat containing receptors; RLRs and NLRs, respectively). For the purposes of this review, we will discuss the uses of liposomes in vaccines that target CLRs and TLRs. The TLRs identified so far amount to 10 in humans, each one recognizing specific PAMPs from microbial pathogens (Table 1 ) [ 10 – 12 ]. TLR 10 has been recently described as a modulatory recep- tor; however, no known ligand has been linked to it [ 13 ]. Therefore, further research should be done on TLR 10 to uncover the ligand involved in innate immune responses. Contrary to the transmembrane TLRs, CLRs are clas- sified as soluble or membrane bound. Soluble CLRs (e.g. galectins and collectins) have been reviewed extensively [ 9 , 14 ]. The mostly studied membrane-associated CLRs are DC-SIGN (DC-specific ICAM3-grabbing non-integ- rin), Dectin-1 (dendritic cell-associated C-type lectin 1), Dectin-2 (dendritic cell-associated C-type lectin 2), MCL (macrophage C-type lectin) and MINCLE (macrophage- inducible C-type lectin) receptors [ 8 , 9 ]. These receptors play a significant role in immunomodulatory responses, triggering the differentiation of T-helper cells (T H cells) from naïve CD4 + T cells, through the assistance of an APC. CLRs not only recognize PAMPs but also the dam- aged-associated molecular patterns (DAMPs) and tumor- associated molecular patterns (TAMPs) from the host [ 15 ] during the processes of apoptosis and tumorigenesis, respectively. Glycans from a myriad of pathogens (para- sitic, fungal, bacterial or viral) are recognized by CLRs (Table 2 ); the most common being mannan [ 16 ], Man- LAM (mannose lipoarabinomannan) [ 17 ], mycobacterial cord factor [ 18 ], β-1,3-glucans [ 8 ] and α-1,2-mannose [ 8 , 19 ]. In humans, DC-SIGN recognizes both mannan and ManLAM; Dectin-1 recognizes β-1,3-glucans and Dec- tin-2 recognizes α-1,2-mannose. In mice, mycobacterial cord factor is recognized by MINCLE and currently no glycans have been identified for the human MINCLE. We can observe from the literature review available, there is still more work to be done to determine ligands or PAMPs that interact with specific PRRs. Scientists must Yüklə 1,05 Mb. Dostları ilə paylaş:
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