construction and preparation of three recombinant adenoviruses expressing truncated ns3 and core genes of hepatitis c virus for vaccine purposes
نویسندگان
چکیده
background in spite of dozens of clinical trials to establish effective therapeutic and/or preventive vaccine to resolve hcv infection, no real vaccine has been proved to date. genetic vaccines based on replication-defective adenoviruses have proved to elicit strong and long lasting t-cell responses against a number of viral antigens and are even currently being used for vaccine trials in humans. according to the controversy in the immune modulatory effects of both core and ns3 full length genes, it seemed more practical to employ some parts of these hcv proteins for vaccine design. objectives to generate recombinant adenoviral vectors containing new overlapping-truncated region of ns3 gene or both the n- and c-terminal deleted parts of core gene, as well as a fusion fragment derived from both of them. materials and methods the corresponding transfer vectors expressing truncated fragments of core, ns3 or a fusion fragment of both genes were prepared. the integrity and sequence of the transfer vectors were confirmed, and followed by experiments involving homologous recombination between them and the adenovirus backbone plasmid in the bacterial host. recombinant ad-pns3, ad-pcore and ad-pns3pcore viruses were prepared by transfection of these new recombined constructs into 293 packaging cell lines. the virus titer was then calculated by an immunohistochemistry based method. the rt-pcr, real-time pcr and western blotting were used to evaluate gene expression by all recombinant constructs. the production of complete virion particles was evaluated by detailed electron microscopy in addition to the appearance of typical cytopathic effects (cpe) and gfp expression patterns in 293 cells. the rt-pcr and gfp detection were employed to monitor the integrity as well as infectivity potency of the viral particles in hep-g2 cells. results rt-pcr, real-time pcr or western blotting confirmed expression of truncated fragment of ns3, core or a fusion fragment of theirs by newly constructed ad-pns3, ad-pcore, ad- pns3pcore particles. electron microscopy, which revealed many adenovirus-like particles and characteristics of cpe in infected cells in addition to gfp detection, confirmed the infectivity, potency and integrity of recombinant adenoviral particles. conclusions these adenoviruses expressing novel fragments of ns3 and core genes may be suitable tools to overcome shortcomings associated with full gene expression in the setting of hcv vaccine therapy.
منابع مشابه
Construction and Preparation of Three Recombinant Adenoviruses Expressing Truncated NS3 and Core Genes of Hepatitis C Virus for Vaccine Purposes
BACKGROUND In spite of dozens of clinical trials to establish effective therapeutic and/or preventive vaccine to resolve HCV infection, no real vaccine has been proved to date. Genetic vaccines based on replication-defective adenoviruses have proved to elicit strong and long lasting T-cell responses against a number of viral antigens and are even currently being used for vaccine trials in human...
متن کاملConstruction of an Expression Vector Containing a Novel Fusion Sequence from Middle Region of NS3 and Truncated Core Genes of Hepatitis C Virus
Background and Aims: DNA constructs containing HCV antigens have become one of the vaccine candidates for induction of anti-HCV cellular and humoral immunity. In this study, we constructed a novel expressing vector harboring a fusion sequence derived from an overlapping fragment in the middle of NS3 and a truncated core fragment to avoid troubles reported to be associated with full gene express...
متن کاملPreparation and characterization of PLGA Nanoparticles containing recombinant core-NS3 Fusion protein of hepatitis C virus as a nano-vaccine candidate
Introduction: Hepatitis C virus (HCV) is one of the most serious causes of cirrhosis, liver cancer and ultimately death, worldwide. The new direct-acting drugs are not accessible for many patients around the world and progress toward new therapeutic and anaphylactic vaccines design has not been fast enough. This study was aimed to prepare and assess a recombinant fusion protein core-NS3 (rC-N) ...
متن کاملConstruction of pIRES2 vector encoding truncated NS3 of HCV and IL-18 for DNA vaccine studies
Introduction: Long term complications of hepatitis C virus (HCV) infection include fibrosis, cirrhosis, and hepatocellular carcinoma and although the disease is treatable with the newly introduced direct acting antivirals, but factors such as drug resistance, viral genotype and adverse effects can limit the effectiveness of therapy. Therefore, development of effective, safe and affordable proph...
متن کاملconstruction and immunogenicity analysis of hepatitis c virus (hcv) truncated non-structural protein 3 (ns3) plasmid vaccine
conclusions the pc-ns3 possesses the capacity to express ns3 in the mammalian cell line and demonstrated strong immunogenicity in a murine model. our primary results demonstrated that the immunogenic truncated region of ns3 could be used as a potential vaccine candidate against hepatitis c. results the pcdna3.1 plasmid harboring the coding sequence of ns3 (pc-ns3) was constructed and confirmed ...
متن کاملconstruction of an expression vector containing a novel fusion sequence from middle region of ns3 and truncated core genes of hepatitis c virus
background and aims: dna constructs containing hcv antigens have become one of the vaccine candidates for induction of anti-hcv cellular and humoral immunity. in this study, we constructed a novel expressing vector harboring a fusion sequence derived from an overlapping fragment in the middle of ns3 and a truncated core fragment to avoid troubles reported to be associated with full gene express...
متن کاملمنابع من
با ذخیره ی این منبع در منابع من، دسترسی به آن را برای استفاده های بعدی آسان تر کنید
عنوان ژورنال:
hepatitis monthlyجلد ۱۲، شماره ۸، صفحات ۰-۰
کلمات کلیدی
میزبانی شده توسط پلتفرم ابری doprax.com
copyright © 2015-2023