Amod Kulkarni
University of Veterinary Medicine and Pharmacy in Kosice, Slovakia
Biography
Nisseria meningitidis casing cererospinal meningitis utilizes several of its membrane proteins to interact with human Brain Microvascular Endothelial Cells (BMECs). Nisseria adhesin A -NadA an outer membrane protein has been recognized to mediate adhesion of bacteria and evokes strong bactericidal antibodies when used as vaccine candidate. In the present study, binding pockets of NadA (domains) interacting with the receptors of BMECs were mapped using mass spectrometry. In brief, binding of BMECs proteins and recombinant NadA (rNadA) expressed in E. coli M15 cells was determined by western blotting. On membrane tryptic digestion (partial) was performed and the non-interacting rNadA fragments were washed to retain BMEC protein-rNadA peptide complex. Further, mild striping was performed on the complex to isolate the domains of rNadA from BMEC proteins. MALDI-TOF/MS was employed to identify the amino acid sequences of the domains. Next, synthetically produced NadA peptides (37 mer peptides) corresponding to the interacting domains of rNadA were used to capture single domain antibodies (VHH) raised against rNadA through M13K07ΔpIII hyper phage system. At least 96 VHH clones were found to have an affinity for rNadA peptide 1 and 2. Among them 20 clones were tested for blocking the interaction of rNadA with BMEC proteins. However, only two clones of VHH binding to globular domain of rNadA and one clone of VHH binding to coiled coil region were able to block the interaction of rNadA with hBMEC proteins.