Abstract
BackgroundChlamydia trachomatis is a human pathogen which causes a number of pathologies, including genital tract infections in women that can result in tubal infertility. Prevention of infection and disease control might be achieved through vaccination; however, a safe, efficacious and cost-effective vaccine against C. trachomatis infection remains an unmet medical need. C. trachomatis major outer membrane protein (MOMP), a β-barrel integral outer membrane protein, is the most abundant antigen in the outer membrane of the bacterium and has been evaluated as a subunit vaccine candidate. Recombinant MOMP (rMOMP) expressed in E. coli cytoplasm forms inclusion bodies and rMOMP extracted from inclusion bodies results in a reduced level of protection compared to the native MOMP in a mouse challenge model.ResultsWe sought to target the recombinant expression of MOMP to the E. coli outer membrane (OM). Successful surface expression was achieved with codon harmonization, utilization of low copy number vectors and promoters with moderate strength, suitable leader sequences and optimization of cell culture conditions. rMOMP was extracted from E. coli outer membrane, purified, and characterized biophysically. The OM expressed and purified rMOMP is immunogenic in mice and elicits antibodies that react to the native antigen, Chlamydia elementary body (EB).ConclusionsC. trachomatis MOMP was functionally expressed on the surface of E. coli outer membrane. The OM expressed and purified rMOMP elicits antibodies that react to the native antigen, Chlamydia EB, in a mouse immunogenicity model. Surface expression of MOMP could provide useful reagents for vaccine research, and the methodology could serve as a platform to produce other outer membrane proteins recombinantly.
Highlights
Chlamydia trachomatis is a human pathogen which causes a number of pathologies, including genital tract infections in women that can result in tubal infertility
Expressed major outer membrane protein (MOMP) has been explored as a vaccine candidate. Recombinant MOMP (rMOMP) expressed without a leader sequence forms inclusion bodies in the cytoplasm of E. coli and rMOMP extracted from inclusion bodies resulted in a reduced level of protection compared to the native MOMP in a mouse challenge model [22, 23]
Refolded rMOMP from E. coli inclusion bodies resulted in a reduced level of protection compared to the native MOMP in a mouse challenge model, suggesting that correct conformation of MOMP is required for protective immune responses [23]
Summary
Chlamydia trachomatis is a human pathogen which causes a number of pathologies, including genital tract infections in women that can result in tubal infertility. Chlamydia trachomatis is an obligate intracellular Gram-negative bacterium responsible for a number of pathologies. Different strains of C. trachomatis are separated into multiple serovars based on serological differences in the Chlamydia major outer membrane protein (MOMP) [1, 2]. C. trachomatis serovars A, B, Ba, and C are responsible for ocular trachoma which can cause conjunctivitis, conjunctival scarring and corneal scarring. Serovars D, Da, E, F, G, H, I, Ia, J, Ja and K are responsible for oculogenital disease which can cause cervicitis, urethritis, endometritis, pelvic inflammatory disease, tubal infertility, ectopic pregnancy, neonatal conjunctivitis and infant pneumonia [3, 4]. A prophylactic vaccine is desirable to prevent C. trachomatis related diseases
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