Aliarcobacter butzleri is an emerging foodborne and zoonotic pathogen, yet many of its encoded proteins remain functionally uncharacterized. This lack of annotation limits understanding of its molecular mechanisms and hampers the identification of novel therapeutic targets. In this study, we systematically performed functional annotation of essential hypothetical proteins from the BNI-3166 strain using an integrative-in-silico approach to uncover potential drug and vaccine candidates. 2,367 protein-coding sequences were retrieved from the RefSeq database and were identified 356 as hypothetical proteins. Using BLASTp, we screened these HPs against the Database of Essential Genes and the human proteome to identify essential non-homologous proteins, resulting in 20 ENH candidates. Functional annotation was performed using several domain-based databases, including Pfam, InterPro, SMART, and SUPERFAMILY. Subsequently, physicochemical properties were analyzed and predicted subcellular localization using PSORTb and CELLO. To assess druggability, the ChEMBL database was used. Virulence factors using VFDB, VICMpred, and VirulentPred 2.0 were also predicted. Gene Ontology annotations were generated via ARGOT2.5. Furthermore, we explored protein-protein interactions using STRING and predicted tertiary structures with AlphaFold3. Moreover, Ligand binding pockets were predicted using PrankWeb, and antigenicity of vaccine candidates was assessed using VaxiJen v2.0. We identified 20 essential non-homologous hypothetical proteins, of which 10 were confidently annotated based on conserved domain analysis. These proteins were classified as enzymes, binding proteins, transporters, regulatory proteins, and potential virulence factors. Among them, eight exhibited characteristics of promising drug targets, while two showed potential as vaccine candidates based on subcellular localization. Druggability analysis revealed that nine proteins had no similarity to known drug targets, suggesting novel therapeutic potential. Predicted 3D structures generated using AlphaFold3 yielded pTM scores ranging from 0.44 to 0.92, indicating acceptable to high modeling confidence. Ligand binding site analysis confirmed druggability in six candidates, and antigenicity screening identified one protein as a potential vaccine target. This study provides a computational framework for identifying functionally important proteins in A. butzleri BNI-3166 and highlights novel therapeutic candidates for experimental validation, offering new directions in drug and vaccine development against this underexplored pathogen.
Key words: Aliarcobacter butzleri, Drug Target Identification, Functional Annotation, Hypothetical Proteins, In Silico Analysis
Received: 08.07.2025; Accepted: 01.09.2025; Early view: 24.09.2025 Published: 10.01.2026
DOI: 10.62063/ecb-66
Citation: Paul, S., Barua, S., & Barua, J.D. (2026). In-silico functional annotation and structural characterization of hypothetical proteins from Aliarcobacter butzleri BNI-3166: Insights into novel virulence and drug targets. The European chemistry and biotechnology journal, 5, 22-39. https://doi.org/10.62063/ecb-66
The copyrights of the studies published in The European Chemistry and Biotechnology Journal (EUCHEMBIOJ) belong to their authors
This article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International (CC BY-NC 4.0)(https://creativecommons.org/licenses/by-nc/4.0/).
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To run Far Cry 4 smoothly on modern Windows systems, users should meet these standards according to System Requirements Lab Recommended Windows 7 (SP1) / 8 / 8.1 (64-bit) Windows 7 (SP1) / 8 / 8.1 (64-bit) Intel Core i5-750 / AMD Phenom II X4 955 Intel Core i7-2600K / AMD FX-8350 NVIDIA GTX 460 / AMD Radeon HD 5850 NVIDIA GTX 680 / AMD Radeon R9 290X Version 11 Version 11 30 GB available space 30 GB available space Troubleshooting Common Issues
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While Version 1.5 was a major fix, the game eventually reached Version 1.10, which added all DLCs (like Valley of the Yetis ) and further refined stability. If you are looking for the absolute most stable version today, newer repacks or the official digital versions on platforms like Steam or Epic Games (which now support ) are often recommended.
To run Far Cry 4 smoothly on modern Windows systems, users should meet these standards according to System Requirements Lab Recommended Windows 7 (SP1) / 8 / 8.1 (64-bit) Windows 7 (SP1) / 8 / 8.1 (64-bit) Intel Core i5-750 / AMD Phenom II X4 955 Intel Core i7-2600K / AMD FX-8350 NVIDIA GTX 460 / AMD Radeon HD 5850 NVIDIA GTX 680 / AMD Radeon R9 290X Version 11 Version 11 30 GB available space 30 GB available space Troubleshooting Common Issues
RG Mechanics is a Russian repacking team known for compressing video games to a fraction of their original size. A "repack" is essentially a cracked version of a game that has been compressed using high-efficiency algorithms (like FreeArc or srep). This makes downloading large titles like Far Cry 4 much faster for users with slower internet connections.