Mehri Habibi - Department of Molecular Biology, Pasteur Institute of Iran, Tehran, Iran
Mohammad Reza Asadi Karam - Department of Molecular Biology, Pasteur Institute of Iran, Tehran, Iran
Saeid Bouzari - Department of Molecular Biology, Pasteur Institute of Iran, Tehran, Iran

Introduction : The innate immune system as the first line of defense against the pathogens recognizes pathogen-associated molecular patterns (PAMPs) by Toll-Like Receptors (TLRs). Interaction of bacterial PAMPs by TLRs results in activation of innate and acquired immunity. FimH adhesin, a minor component of type ۱ fimbriae encoded by Uropathogenic Escherichia coli (UPEC) is a PAMP of TLR۴ that stimulates the innate immunity against infections. The FimH involves N-terminal and C-terminal domains. Detailed information about the TLR۴ interaction with FimH is lacking. Methods: In this study, we evaluated interaction between TLR۴ and whole FimH and two domains of FimH using computational methods. Two truncated forms of FimH that included N- terminal and C- terminal truncated forms were selected from PDB. Molecular docking analysis of TLR۴ against FimH was done using HEX docking tool. The molecular interaction plot between TLR۴ and FimH was generated Dimplot in LIGPLOT software (v. ۴.۵.۳). Results: Based on the total free energy, C- terminal truncated form had the best interaction tendency to the receptor. Dimplot analysis showed that there are ۱۱ intermolecular hydrogen bonds in the TLR۴ and C- terminal truncated form of FimH complex. Conclusion: The high affinity of C- terminal truncated form to TLR۴ suggests that this portion of FimH has important effect on the adjuvant activity and innate immune response and could utilize as adjuvant for vaccine application against microbial infections and cancers. J Med Microbiol Infec Dis, ۲۰۱۴, ۱ (۲): ۵ pages.

Toll-Like Receptors, FimH, Truncated form, Molecular Docking Analysis