N-Linked Glycosylation at an Appropriate Position in the Pre-S2 Domain Is Critical for Cellular and Humoral Immunity against Middle HBV Surface Antigen

Líu, Hao; Wang, Shixia; Jia, Yiqiong; Li, Jun; Huang, Zhibin; Lu, Shan; Xing, Yiping

doi:10.1620/tjem.236.131

Cited by 2 publications

(1 citation statement)

References 29 publications

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“…Removal of the conserved preS2 N-linked glycan of the M protein had deleterious effects on both virus particles and M-SVPs [ 11 ]. Moreover, N4 glycosylation was later shown to be a crucial determinant of the M-based DNA vaccine efficiency [ 51 ]. Therefore, studying an M protein with altered rather than absent N-linked glycans was an alternative approach to further optimize the antigenic features of this immunogen.…”

Section: Hbv N-glycosylation and The Interaction With The Host Immmentioning

confidence: 99%

N-Glycosylation and N-Glycan Processing in HBV Biology and Pathogenesis

Dobrica

Lazar

Branza‐Nichita

2020

Cells

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Hepatitis B Virus (HBV) glycobiology has been an area of intensive research in the last decades and continues to be an attractive topic due to the multiple roles that N-glycosylation in particular plays in the virus life-cycle and its interaction with the host that are still being discovered. The three HBV envelope glycoproteins, small (S), medium (M) and large (L) share a very peculiar N-glycosylation pattern, which distinctly regulates their folding, degradation, assembly, intracellular trafficking and antigenic properties. In addition, recent findings indicate important roles of N-linked oligosaccharides in viral pathogenesis and evasion of the immune system surveillance. This review focuses on N-glycosylation’s contribution to HBV infection and disease, with implications for development of improved vaccines and antiviral therapies.

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Section: Hbv N-glycosylation and The Interaction With The Host Immmentioning

confidence: 99%

N-Glycosylation and N-Glycan Processing in HBV Biology and Pathogenesis

Dobrica

Lazar

Branza‐Nichita

2020

Cells

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A design space exploration for control of Critical Quality Attributes of mAb

Bhatia

Read

Agarabi

et al. 2016

International Journal of Pharmaceutics

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A unique "design space (DSp) exploration strategy," defined as a function of four key scenarios, was successfully integrated and validated to enhance the DSp building exercise, by increasing the accuracy of analyses and interpretation of processed data. The four key scenarios, defining the strategy, were based on cumulative analyses of individual models developed for the Critical Quality Attributes (23 Glycan Profiles) considered for the study. The analyses of the CQA estimates and model performances were interpreted as (1) Inside Specification/Significant Model (2) Inside Specification/Non-significant Model (3) Outside Specification/Significant Model (4) Outside Specification/Non-significant Model. Each scenario was defined and illustrated through individual models of CQA aligning the description. The R(2), Q(2), Model Validity and Model Reproducibility estimates of G2, G2FaGbGN, G0 and G2FaG2, respectively, signified the four scenarios stated above. Through further optimizations, including the estimation of Edge of Failure and Set Point Analysis, wider and accurate DSps were created for each scenario, establishing critical functional relationship between Critical Process Parameters (CPPs) and Critical Quality Attributes (CQAs). A DSp provides the optimal region for systematic evaluation, mechanistic understanding and refining of a QbD approach. DSp exploration strategy will aid the critical process of consistently and reproducibly achieving predefined quality of a product throughout its lifecycle.

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N-Linked Glycosylation at an Appropriate Position in the Pre-S2 Domain Is Critical for Cellular and Humoral Immunity against Middle HBV Surface Antigen

Cited by 2 publications

References 29 publications

N-Glycosylation and N-Glycan Processing in HBV Biology and Pathogenesis

N-Glycosylation and N-Glycan Processing in HBV Biology and Pathogenesis

A design space exploration for control of Critical Quality Attributes of mAb

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