Search

Your search keyword '"Benkahla A"' showing total 394 results
Start Over Author "Benkahla A" Search Limiters Full Text
394 results on '"Benkahla A"'

1. Genome Tunisia Project: paving the way for precision medicine in North Africa

Author

Hamdi, Yosr, Trabelsi, Mediha, Ghedira, Kais, Boujemaa, Maroua, Ben Ayed, Ikhlas, Charfeddine, Cherine, Souissi, Amal, Rejeb, Imen, Kammoun Rebai, Wafa, Hkimi, Chaima, Neifar, Fadoua, Jandoubi, Nouha, Mkaouar, Rahma, Chaouch, Melek, Bennour, Ayda, Kamoun, Selim, Chaker Masmoudi, Hend, Abid, Nabil, Mezghani Khemakhem, Maha, Masmoudi, Saber, Saad, Ali, BenJemaa, Lamia, BenKahla, Alia, Boubaker, Samir, Mrad, Ridha, Kamoun, Hassen, Abdelhak, Sonia, Gribaa, Moez, Belguith, Neila, Kharrat, Najla, Hmida, Dorra, and Rebai, Ahmed

Published
2024
Full Text
View/download PDF

2. Genome Tunisia Project: paving the way for precision medicine in North Africa

Author

Yosr Hamdi, Mediha Trabelsi, Kais Ghedira, Maroua Boujemaa, Ikhlas Ben Ayed, Cherine Charfeddine, Amal Souissi, Imen Rejeb, Wafa Kammoun Rebai, Chaima Hkimi, Fadoua Neifar, Nouha Jandoubi, Rahma Mkaouar, Melek Chaouch, Ayda Bennour, Selim Kamoun, Hend Chaker Masmoudi, Nabil Abid, Maha Mezghani Khemakhem, On behalf of the GTCA Consortium, Saber Masmoudi, Ali Saad, Lamia BenJemaa, Alia BenKahla, Samir Boubaker, Ridha Mrad, Hassen Kamoun, Sonia Abdelhak, Moez Gribaa, Neila Belguith, Najla Kharrat, Dorra Hmida, and Ahmed Rebai

Subjects
Tunisian reference genome, Precision medicine, Human genomics, Socio-economic impact, Data sharing, Government support, Medicine, Genetics, QH426-470
Abstract

Abstract Background Key discoveries and innovations in the field of human genetics have led to the foundation of molecular and personalized medicine. Here, we present the Genome Tunisia Project, a two-phased initiative (2022–2035) which aims to deliver the reference sequence of the Tunisian Genome and to support the implementation of personalized medicine in Tunisia, a North African country that represents a central hub of population admixture and human migration between African, European, and Asian populations. The main goal of this initiative is to develop a healthcare system capable of incorporating omics data for use in routine medical practice, enabling medical doctors to better prevent, diagnose, and treat patients. Methods A multidisciplinary partnership involving Tunisian experts from different institutions has come to discern all requirements that would be of high priority to fulfill the project’s goals. One of the most urgent priorities is to determine the reference sequence of the Tunisian Genome. In addition, extensive situation analysis and revision of the education programs, community awareness, appropriate infrastructure including sequencing platforms and biobanking, as well as ethical and regulatory frameworks, have been undertaken towards building sufficient capacity to integrate personalized medicine into the Tunisian healthcare system. Results In the framework of this project, an ecosystem with all engaged stakeholders has been implemented including healthcare providers, clinicians, researchers, pharmacists, bioinformaticians, industry, policymakers, and advocacy groups. This initiative will also help to reinforce research and innovation capacities in the field of genomics and to strengthen discoverability in the health sector. Conclusions Genome Tunisia is the first initiative in North Africa that seeks to demonstrate the major impact that can be achieved by Human Genome Projects in low- and middle-income countries to strengthen research and to improve disease management and treatment outcomes, thereby reducing the social and economic burden on healthcare systems. Sharing this experience within the African scientific community is a chance to turn a major challenge into an opportunity for dissemination and outreach. Additional efforts are now being made to advance personalized medicine in patient care by educating consumers and providers, accelerating research and innovation, and supporting necessary changes in policy and regulation.

Published
2024
Full Text
View/download PDF

3. Recombination Events Among SARS-CoV-2 Omicron Subvariants: Impact on Spike Interaction With ACE2 Receptor and Neutralizing Antibodies

Author

Marwa Arbi, Marwa Khedhiri, Kaouther Ayouni, Oussema Souiai, Samar Dhouib, Nidhal Ghanmi, Alia Benkahla, Henda Triki, and Sondes Haddad-Boubaker

Subjects
Evolution, QH359-425
Abstract

The recombination plays a key role in promoting evolution of RNA viruses and emergence of potentially epidemic variants. Some studies investigated the recombination occurrence among SARS-CoV-2, without exploring its impact on virus-host interaction. In the aim to investigate the burden of recombination in terms of frequency and distribution, the occurrence of recombination was first explored in 44 230 Omicron sequences among BQ subvariants and the under investigation “ML” (Multiple Lineages) denoted sequences, using 3seq software. Second, the recombination impact on interaction between the Spike protein and ACE2 receptor as well as neutralizing antibodies (nAbs), was analyzed using docking tools. Recombination was detected in 56.91% and 82.20% of BQ and ML strains, respectively. It took place mainly in spike and ORF1a genes. For BQ recombinant strains, the docking analysis showed that the spike interacted strongly with ACE2 and weakly with nAbs. The mutations S373P, S375F and T376A constitute a residue network that enhances the RBD interaction with ACE2. Thirteen mutations in RBD (S373P, S375F, T376A, D405N, R408S, K417N, N440K, S477N, P494S, Q498R, N501Y, and Y505H) and NTD (Y240H) seem to be implicated in immune evasion of recombinants by altering spike interaction with nAbs. In conclusion, this “in silico” study demonstrated that the recombination mechanism is frequent among Omicron BQ and ML variants. It highlights new key mutations, that potentially implicated in enhancement of spike binding to ACE2 (F376A) and escape from nAbs (RBD: F376A, D405N, R408S, N440K, S477N, P494S, and Y505H; NTD: Y240H). Our findings present considerable insights for the elaboration of effective prophylaxis and therapeutic strategies against future SARS-CoV-2 waves.

Published
2024
Full Text
View/download PDF

4. Methodology optimizing SAGE library tag-to-gene mapping: application to Leishmania

Author

Smandi Sondos, Guerfali Fatma Z, Farhat Mohamed, Ben-Aissa Khadija, Laouini Dhafer, Guizani-Tabbane Lamia, Dellagi Koussay, and Benkahla Alia

Subjects
Medicine, Biology (General), QH301-705.5, Science (General), Q1-390
Abstract

Abstract Background Leishmaniasis are widespread parasitic-diseases with an urgent need for more active and less toxic drugs and for effective vaccines. Understanding the biology of the parasite especially in the context of host parasite interaction is a crucial step towards such improvements in therapy and control. Several experimental approaches including SAGE (Serial analysis of gene expression) have been developed in order to investigate the parasite transcriptome organisation and plasticity. Usual SAGE tag-to-gene mapping techniques are inadequate because almost all tags are normally located in the 3'-UTR outside the CDS, whereas most information available for Leishmania transcripts is restricted to the CDS predictions. The aim of this work is to optimize a SAGE libraries tag-to-gene mapping technique and to show how this development improves the understanding of Leishmania transcriptome. Findings The in silico method implemented herein was based on mapping the tags to Leishmania genome using BLAST then mapping the tags to their gene using a data-driven probability distribution. This optimized tag-to-gene mappings improved the knowledge of Leishmania genome structure and transcription. It allowed analyzing the expression of a maximal number of Leishmania genes, the delimitation of the 3' UTR of 478 genes and the identification of biological processes that are differentially modulated during the promastigote to amastigote differentiation. Conclusion The developed method optimizes the assignment of SAGE tags in trypanosomatidae genomes as well as in any genome having polycistronic transcription and small intergenic regions.

Published
2012
Full Text
View/download PDF

5. Basal DNA repair machinery is subject to positive selection in ionizing-radiation-resistant bacteria

Author

Barkallah Insaf, Benkahla Alia, Ghedira Kaïs, and Sghaier Haïtham

Subjects
Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Ionizing-radiation-resistant bacteria (IRRB) show a surprising capacity for adaptation to ionizing radiation and desiccation. Positive Darwinian selection is expected to play an important role in this trait, but no data are currently available regarding the role of positive adaptive selection in resistance to ionizing-radiation and tolerance of desiccation. We analyzed the four known genome sequences of IRRB (Deinococcus geothermalis, Deinococcus radiodurans, Kineococcus radiotolerans, and Rubrobacter xylanophilus) to determine the role of positive Darwinian selection in the evolution of resistance to ionizing radiation and tolerance of desiccation. Results We used the programs MultiParanoid and DnaSP to deduce the sets of orthologs that potentially evolved due to positive Darwinian selection in IRRB. We find that positive selection targets 689 ortholog sets of IRRB. Among these, 58 ortholog sets are absent in ionizing-radiation-sensitive bacteria (IRSB: Escherichia coli and Thermus thermophilus). The most striking finding is that all basal DNA repair genes in IRRB, unlike many of their orthologs in IRSB, are subject to positive selection. Conclusion Our results provide the first in silico prediction of positively selected genes with potential roles in the molecular basis of resistance to γ-radiation and tolerance of desiccation in IRRB. Identification of these genes provides a basis for future experimental work aimed at understanding the metabolic networks in which they participate.

Published
2008
Full Text
View/download PDF

6. Simultaneous gene expression profiling in human macrophages infected with Leishmania major parasites using SAGE

Author

Smandi Sondos, Manchon Laurent, Piquemal David, Benkahla Alia, Ben-Aissa Khadija, Ottones Florence, Guizani-Tabbane Lamia, Laouini Dhafer, Guerfali Fatma Z, Mghirbi Ons, Commes Thérèse, Marti Jacques, and Dellagi Koussay

Subjects
Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Leishmania (L) are intracellular protozoan parasites that are able to survive and replicate within the harsh and potentially hostile phagolysosomal environment of mammalian mononuclear phagocytes. A complex interplay then takes place between the macrophage (MΦ) striving to eliminate the pathogen and the parasite struggling for its own survival. To investigate this host-parasite conflict at the transcriptional level, in the context of monocyte-derived human MΦs (MDM) infection by L. major metacyclic promastigotes, the quantitative technique of serial analysis of gene expression (SAGE) was used. Results After extracting mRNA from resting human MΦs, Leishmania-infected human MΦs and L. major parasites, three SAGE libraries were constructed and sequenced generating up to 28,173; 57,514 and 33,906 tags respectively (corresponding to 12,946; 23,442 and 9,530 unique tags). Using computational data analysis and direct comparison to 357,888 publicly available experimental human tags, the parasite and the host cell transcriptomes were then simultaneously characterized from the mixed cellular extract, confidently discriminating host from parasite transcripts. This procedure led us to reliably assign 3,814 tags to MΦs' and 3,666 tags to L. major parasites transcripts. We focused on these, showing significant changes in their expression that are likely to be relevant to the pathogenesis of parasite infection: (i) human MΦs genes, belonging to key immune response proteins (e.g., IFNγ pathway, S100 and chemokine families) and (ii) a group of Leishmania genes showing a preferential expression at the parasite's intra-cellular developing stage. Conclusion Dual SAGE transcriptome analysis provided a useful, powerful and accurate approach to discriminating genes of human or parasitic origin in Leishmania-infected human MΦs. The findings presented in this work suggest that the Leishmania parasite modulates key transcripts in human MΦs that may be beneficial for its establishment and survival. Furthermore, these results provide an overview of gene expression at two developmental stages of the parasite, namely metacyclic promastigotes and intracellular amastigotes and indicate a broad difference between their transcriptomic profiles. Finally, our reported set of expressed genes will be useful in future rounds of data mining and gene annotation.

Published
2008
Full Text
View/download PDF

7. Retrospective Phylodynamic and Phylogeographic Analysis of the Bluetongue Virus in Tunisia

Author

Oussema Souiai, Marwa Arbi, Mariem Hanachi, Ameny Sallami, Imen Larbi, Melek Chaouch, Emna Harigua-Souiai, and Alia Benkahla

Subjects
Evolution, QH359-425
Abstract

Bluetongue virus (BTV) is an arbovirus considered as a major threat for the global livestock economy. Since 1999, Tunisia has experienced several incursions of BTV, during which numerous cases of infection and mortality have been reported. However, the geographical origin and epidemiological characteristics of these incursions remained unclear. To understand the evolutionary history of BTV emergence in Tunisia, we extracted from Genbank the segment 6 sequences of 7 BTV strains isolated in Tunisia during the period 2000 to 2017 and blasted them to obtain a final dataset of 67 sequences. We subjected the dataset to a Bayesian phylogeography framework inferring geographical origin and serotype as phylodynamic models. Our results suggest that BTV-2 was first introduced in Tunisia in the 1960s and that since 1990s, the country has witnessed the emergence of other typical and atypical BTV serotypes notably BTV-1, BTV-3 and BTV-Y. The reported serotypes have a diverse geographical origin and have been transmitted to Tunisia from countries in the Mediterranean Basin. Interserotype reassortments have been identified among BTV-1, BTV-2 and BTV-Y. This study has provided new insights on the temporal and geographical origin of BTV in Tunisia, suggesting the contribution of animal trade and environment conditions in virus spread.

Published
2023
Full Text
View/download PDF

8. Cross-species hybridisation of human and bovine orthologous genes on high density cDNA microarrays

Author

Hultschig Claus, Carnwath Joseph W, Nowak Monika, Brink Thore C, BenKahla Alia, Wruck Wasco, Herrmann Doris, Herwig Ralf, Adjaye James, Niemann Heiner, and Lehrach Hans

Subjects
Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Cross-species gene-expression comparison is a powerful tool for the discovery of evolutionarily conserved mechanisms and pathways of expression control. The usefulness of cDNA microarrays in this context is that broad areas of homology are compared and hybridization probes are sufficiently large that small inter-species differences in nucleotide sequence would not affect the analytical results. This comparative genomics approach would allow a common set of genes within a specific developmental, metabolic, or disease-related gene pathway to be evaluated in experimental models of human diseases. The objective of this study was to investigate the feasibility and reproducibility of cross-species analysis employing a human cDNA microarray as probe. Results As a proof of principle, total RNA derived from human and bovine fetal brains was used as a source of labelled targets for hybridisation onto a human cDNA microarray composed of 349 characterised genes. Each gene was spotted 20 times representing 6,980 data points thus enabling highly reproducible spot quantification. Employing high stringency hybridisation and washing conditions, followed by data analysis, revealed slight differences in the expression levels and reproducibility of the signals between the two species. We also assigned each of the genes into three expression level categories- i.e. high, medium and low. The correlation co-efficient of cross hybridisation between the orthologous genes was 0.94. Verification of the array data by semi-quantitative RT-PCR using common primer sequences enabled co-amplification of both human and bovine transcripts. Finally, we were able to assign gene names to previously uncharacterised bovine ESTs. Conclusions Results of our study demonstrate the harnessing and utilisation power of comparative genomics and prove the feasibility of using human microarrays to facilitate the identification of co-expressed orthologous genes in common tissues derived from different species.

Published
2004
Full Text
View/download PDF

9. Vemurafenib Inhibits Acute and Chronic Enterovirus Infection by Affecting Cellular Kinase Phosphatidylinositol 4-Kinase Type IIIβ

Author

Mira Laajala, Marleen Zwaagstra, Mari Martikainen, Magloire Pandoua Nekoua, Mehdi Benkahla, Famara Sane, Emily Gervais, Grace Campagnola, Anni Honkimaa, Amir-Babak Sioofy-Khojine, Heikki Hyöty, Ravi Ojha, Marie Bailliot, Giuseppe Balistreri, Olve Peersen, Didier Hober, Frank Van Kuppeveld, and Varpu Marjomäki

Subjects
acute infection, antiviral, chronic infection, drug repurposing, enterovirus, Microbiology, QR1-502
Abstract

ABSTRACT Enteroviruses are one of the most abundant viruses causing mild to serious acute infections in humans and also contributing to chronic diseases like type 1 diabetes. Presently, there are no approved antiviral drugs against enteroviruses. Here, we studied the potency of vemurafenib, an FDA-approved RAF kinase inhibitor for treating BRAFV600E mutant-related melanoma, as an antiviral against enteroviruses. We showed that vemurafenib prevented enterovirus translation and replication at low micromolar dosage in an RAF/MEK/ERK-independent manner. Vemurafenib was effective against group A, B, and C enteroviruses, as well as rhinovirus, but not parechovirus or more remote viruses such as Semliki Forest virus, adenovirus, and respiratory syncytial virus. The inhibitory effect was related to a cellular phosphatidylinositol 4-kinase type IIIβ (PI4KB), which has been shown to be important in the formation of enteroviral replication organelles. Vemurafenib prevented infection efficiently in acute cell models, eradicated infection in a chronic cell model, and lowered virus amounts in pancreas and heart in an acute mouse model. Altogether, instead of acting through the RAF/MEK/ERK pathway, vemurafenib affects the cellular PI4KB and, hence, enterovirus replication, opening new possibilities to evaluate further the potential of vemurafenib as a repurposed drug in clinical care. IMPORTANCE Despite the prevalence and medical threat of enteroviruses, presently, there are no antivirals against them. Here, we show that vemurafenib, an FDA-approved RAF kinase inhibitor for treating BRAFV600E mutant-related melanoma, prevents enterovirus translation and replication. Vemurafenib shows efficacy against group A, B, and C enteroviruses, as well as rhinovirus, but not parechovirus or more remote viruses such as Semliki Forest virus, adenovirus, and respiratory syncytial virus. The inhibitory effect acts through cellular phosphatidylinositol 4-kinase type IIIβ (PI4KB), which has been shown to be important in the formation of enteroviral replication organelles. Vemurafenib prevents infection efficiently in acute cell models, eradicates infection in a chronic cell model, and lowers virus amounts in pancreas and heart in an acute mouse model. Our findings open new possibilities to develop drugs against enteroviruses and give hope for repurposing vemurafenib as an antiviral drug against enteroviruses.

Published
2023
Full Text
View/download PDF

10. A linear algorithm for computing Polynomial Dynamical System

Author

Abdeljaoued-Tej, Ines, BenKahla, Alia, Haddad, Ghassen, and Valibouze, Annick

Subjects
Quantitative Biology - Molecular Networks, Mathematics - Optimization and Control
Abstract

Computation biology helps to understand all processes in organisms from interaction of molecules to complex functions of whole organs. Therefore, there is a need for mathematical methods and models that deliver logical explanations in a reasonable time. For the last few years there has been a growing interest in biological theory connected to finite fields: the algebraic modeling tools used up to now are based on Gr\"obner bases or Boolean group. Let $n$ variables representing gene products, changing over the time on $p$ values. A Polynomial dynamical system (PDS) is a function which has several components, each one is a polynom with $n$ variables and coefficient in the finite field $Z/pZ$ that model the evolution of gene products. We propose herein a method using algebraic separators, which are special polynomials abundantly studied in effective Galois theory. This approach avoids heavy calculations and provides a first Polynomial model in linear time., Comment: 11 pages, 3 figures

Published
2018

11. Host M-CSF induced gene expression drives changes in susceptible and resistant mice-derived BMdMs upon Leishmania major infection

Author

Cyrine Bouabid, Sameh Rabhi, Kristina Thedinga, Gal Barel, Hedia Tnani, Imen Rabhi, Alia Benkahla, Ralf Herwig, and Lamia Guizani-Tabbane

Subjects
macrophages, M-CSF, host background, Resistance, susceptibility, transcriptome, Immunologic diseases. Allergy, RC581-607
Abstract

Leishmaniases are a group of diseases with different clinical manifestations. Macrophage-Leishmania interactions are central to the course of the infection. The outcome of the disease depends not only on the pathogenicity and virulence of the parasite, but also on the activation state, the genetic background, and the underlying complex interaction networks operative in the host macrophages. Mouse models, with mice strains having contrasting behavior in response to parasite infection, have been very helpful in exploring the mechanisms underlying differences in disease progression. We here analyzed previously generated dynamic transcriptome data obtained from Leishmania major (L. major) infected bone marrow derived macrophages (BMdMs) from resistant and susceptible mouse. We first identified differentially expressed genes (DEGs) between the M-CSF differentiated macrophages derived from the two hosts, and found a differential basal transcriptome profile independent of Leishmania infection. These host signatures, in which 75% of the genes are directly or indirectly related to the immune system, may account for the differences in the immune response to infection between the two strains. To gain further insights into the underlying biological processes induced by L. major infection driven by the M-CSF DEGs, we mapped the time-resolved expression profiles onto a large protein-protein interaction (PPI) network and performed network propagation to identify modules of interacting proteins that agglomerate infection response signals for each strain. This analysis revealed profound differences in the resulting responses networks related to immune signaling and metabolism that were validated by qRT-PCR time series experiments leading to plausible and provable hypotheses for the differences in disease pathophysiology. In summary, we demonstrate that the host’s gene expression background determines to a large degree its response to L. major infection, and that the gene expression analysis combined with network propagation is an effective approach to help identifying dynamically altered mouse strain-specific networks that hold mechanistic information about these contrasting responses to infection.

Published
2023
Full Text
View/download PDF

12. Antibody escape and global spread of SARS-CoV-2 lineage A.27

Author

Kaleta, Tamara, Kern, Lisa, Hong, Samuel Leandro, Hölzer, Martin, Kochs, Georg, Beer, Julius, Schnepf, Daniel, Schwemmle, Martin, Bollen, Nena, Kolb, Philipp, Huber, Magdalena, Ulferts, Svenja, Weigang, Sebastian, Dudas, Gytis, Wittig, Alice, Jaki, Lena, Padane, Abdou, Lagare, Adamou, Salou, Mounerou, Ozer, Egon Anderson, Nnaemeka, Ndodo, Odoom, John Kofi, Rutayisire, Robert, Benkahla, Alia, Akoua-Koffi, Chantal, Ouedraogo, Abdoul-Salam, Simon-Lorière, Etienne, Enouf, Vincent, Kröger, Stefan, Calvignac-Spencer, Sébastien, Baele, Guy, Panning, Marcus, and Fuchs, Jonas

Published
2022
Full Text
View/download PDF

14. Developing Clinical Phenotype Data Collection Standards for Research in Africa

Author

Lyndon Zass, Katherine Johnston, Alia Benkahla, Melek Chaouch, Judit Kumuthini, Fouzia Radouani, Liberata Alexander Mwita, Nihad Alsayed, Taryn Allie, Dassen Sathan, Upendo Masamu, Milaine Sergine Seuneu Tchamga, Tsaone Tamuhla, Chaimae Samtal, Victoria Nembaware, Zoe Gill, Samah Ahmed, Yosr Hamdi, Faisal Fadlelmola, Nicki Tiffin, and Nicola Mulder

Subjects
Public aspects of medicine, RA1-1270
Abstract

Modern biomedical research is characterised by its high-throughput and interdisciplinary nature. Multiproject and consortium-based collaborations requiring meaningful analysis of multiple heterogeneous phenotypic datasets have become the norm; however, such analysis remains a challenge in many regions across the world. An increasing number of data harmonisation efforts are being undertaken by multistudy collaborations through either prospective standardised phenotype data collection or retrospective phenotype harmonisation. In this regard, the Phenotype Harmonisation Working Group (PHWG) of the Human Heredity and Health in Africa (H3Africa) consortium aimed to facilitate phenotype standardisation by both promoting the use of existing data collection standards (hosted by PhenX), adapting existing data collection standards for appropriate use in low- and middle-income regions such as Africa, and developing novel data collection standards where relevant gaps were identified. Ultimately, the PHWG produced 11 data collection kits, consisting of 82 protocols, 38 of which were existing protocols, 17 were adapted, and 27 were novel protocols. The data collection kits will facilitate phenotype standardisation and harmonisation not only in Africa but also across the larger research community. In addition, the PHWG aims to feed back adapted and novel protocols to existing reference platforms such as PhenX.

Published
2023
Full Text
View/download PDF

16. New neural network classification method for individuals ancestry prediction from SNPs data

Author

H. Soumare, S. Rezgui, N. Gmati, and A. Benkahla

Subjects
Artificial neural network, Dimensionality reduction, Input perturbation, Single nucleotide polymorphism, Singular value decomposition, Computer applications to medicine. Medical informatics, R858-859.7, Analysis, QA299.6-433
Abstract

Abstract Artificial Neural Network (ANN) algorithms have been widely used to analyse genomic data. Single Nucleotide Polymorphisms(SNPs) represent the genetic variations, the most common in the human genome, it has been shown that they are involved in many genetic diseases, and can be used to predict their development. Developing ANN to handle this type of data can be considered as a great success in the medical world. However, the high dimensionality of genomic data and the availability of a limited number of samples can make the learning task very complicated. In this work, we propose a New Neural Network classification method based on input perturbation. The idea is first to use SVD to reduce the dimensionality of the input data and to train a classification network, which prediction errors are then reduced by perturbing the SVD projection matrix. The proposed method has been evaluated on data from individuals with different ancestral origins, the experimental results have shown the effectiveness of the proposed method. Achieving up to 96.23% of classification accuracy, this approach surpasses previous Deep learning approaches evaluated on the same dataset.

Published
2021
Full Text
View/download PDF

17. In silico prediction of protein-protein interactions in human macrophages

Author

Souiai, Oussema, Guerfali, Fatma, Miled, Slimane Ben, Brun, Christine, and Benkahla, Alia

Subjects
Quantitative Biology - Molecular Networks
Abstract

Background: Protein-protein interaction (PPI) network analyses are highly valuable in deciphering and understanding the intricate organisation of cellular functions. Nevertheless, the majority of available protein-protein interaction networks are context-less, i.e. without any reference to the spatial, temporal or physiological conditions in which the interactions may occur. In this work, we are proposing a protocol to infer the most likely protein-protein interaction (PPI) network in human macrophages. Results: We integrated the PPI dataset from the Agile Protein Interaction DataAnalyzer (APID) with different meta-data to infer a contextualized macrophage-specific interactome using a combination of statistical methods. The obtained interactome is enriched in experimentally verified interactions and in proteins involved in macrophage-related biological processes (i.e. immune response activation, regulation of apoptosis). As a case study, we used the contextualized interactome to highlight the cellular processes induced upon Mycobacterium tuberculosis infection. Conclusion: Our work confirms that contextualizing interactomes improves the biological significance of bioinformatic analyses. More specifically, studying such inferred network rather than focusing at the gene expression level only, is informative on the processes involved in the host response. Indeed, important immune features such as apoptosis are solely highlighted when the spotlight is on the protein interaction level.

Published
2015
Full Text
View/download PDF

18. Recombination Events Among SARS-CoV-2 Omicron Subvariants: Impact on Spike Interaction With ACE2 Receptor and Neutralizing Antibodies.

Author

Arbi, Marwa, Khedhiri, Marwa, Ayouni, Kaouther, Souiai, Oussema, Dhouib, Samar, Ghanmi, Nidhal, Benkahla, Alia, Triki, Henda, and Haddad-Boubaker, Sondes

Subjects
SARS-CoV-2 Omicron variant, RNA viruses, ANGIOTENSIN converting enzyme, RECEPTOR antibodies, PROTEIN receptors
Abstract

The recombination plays a key role in promoting evolution of RNA viruses and emergence of potentially epidemic variants. Some studies investigated the recombination occurrence among SARS-CoV-2, without exploring its impact on virus-host interaction. In the aim to investigate the burden of recombination in terms of frequency and distribution, the occurrence of recombination was first explored in 44 230 Omicron sequences among BQ subvariants and the under investigation "ML" (Multiple Lineages) denoted sequences, using 3seq software. Second, the recombination impact on interaction between the Spike protein and ACE2 receptor as well as neutralizing antibodies (nAbs), was analyzed using docking tools. Recombination was detected in 56.91% and 82.20% of BQ and ML strains, respectively. It took place mainly in spike and ORF1a genes. For BQ recombinant strains, the docking analysis showed that the spike interacted strongly with ACE2 and weakly with nAbs. The mutations S373P, S375F and T376A constitute a residue network that enhances the RBD interaction with ACE2. Thirteen mutations in RBD (S373P, S375F, T376A, D405N, R408S, K417N, N440K, S477N, P494S, Q498R, N501Y, and Y505H) and NTD (Y240H) seem to be implicated in immune evasion of recombinants by altering spike interaction with nAbs. In conclusion, this "in silico" study demonstrated that the recombination mechanism is frequent among Omicron BQ and ML variants. It highlights new key mutations, that potentially implicated in enhancement of spike binding to ACE2 (F376A) and escape from nAbs (RBD: F376A, D405N, R408S, N440K, S477N, P494S, and Y505H; NTD: Y240H). Our findings present considerable insights for the elaboration of effective prophylaxis and therapeutic strategies against future SARS-CoV-2 waves. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

19. Natural Convection of Power Law Fluid through a Porous Deposit: MRT-LBM Approach

Author

A. Bourada, A. Boutra, K. Bouarnouna, D. E. Ameziani, and Y. K. Benkahla

Subjects
modified darcy-brinkman model, square cavity, semi-cylinder., Mechanical engineering and machinery, TJ1-1570
Abstract

In this research, natural convection of power law fluid in a square cavity, with a porous deposit in the shape of a semi-cylinder is studied numerically, using the multiple-relaxation-time lattice Boltzmann method. The modified Darcy-Brinkman model is applied for modelling the momentum equations in porous medium and the Boussinesq assumption is adopted to model the buoyancy force term. The influences of power law index (0.6 ≤ n ≤ 1.4), Darcy number (10−5 ≤ Da ≤ 10−2), Rayleigh number (103 ≤ Ra ≤ 106) and the radius ratio of the semi-cylindrical porous deposit (0.05 ≤ R ≤ 0.5) on hydrodynamic and heat transfer are studied. The obtained results show that these parameters have an important effect, on the structure of hydrodynamic and thermal transfer. The improvement of the power law index leads to a decrease in the heat transfer rate, illustrated by the average Nusselt number, and the augmentation in Darcy number induces an increase in that rate. Moreover, the variation of the Rayleigh number and the porous deposit radius has a significant effect on the transfer rate and convective structure. Besides, an unusual phenomenon is noticed for high Rayleigh numbers, where a better heat evacuation from the porous deposit is noticed for the dilatant fluid compared to the pseudoplastic one.

Published
2021

20. Longitudinal and Comparative Analysis of Gut Microbiota of Tunisian Newborns According to Delivery Mode

Author

Mariem Hanachi, Olfa Maghrebi, Haifa Bichiou, Ferdaous Trabelsi, Najla Maha Bouyahia, Fethi Zhioua, Meriam Belghith, Emna Harigua-Souiai, Meriem Baouendi, Lamia Guizani-Tabbane, Alia Benkahla, and Oussema Souiai

Subjects
shotgun metagenome sequencing, newborns, elective cesarean deliveries, ESKAPE bacteria, Tunisia, microbiome, Microbiology, QR1-502
Abstract

Microbiota colonization is a dynamic process that impacts the health status during an individual's lifetime. The composition of the gut microbiota of newborns is conditioned by multiple factors, including the delivery mode (DM). Nonetheless, the DM's influence remains uncertain and is still the subject of debate. In this context, the medical indication and the emergency of a cesarean delivery might have led to confounding conclusions regarding the composition and diversity of the neonatal microbiome. Herein, we used high-resolution shotgun sequencing to decipher the composition and dynamics of the gut microbiota composition of Tunisian newborns. Stool samples were collected from 5 elective cesarean section (ECS) and 5 vaginally delivered (VD) newborns at the following time points: Day 0, Day 15, and Day 30. The ECS and VD newborns showed the same level of bacterial richness and diversity. In addition, our data pointed to a shift in microbiota community composition during the first 2 weeks, regardless of the DM. Both ECS and VD showed a profile dominated by Proteobacteria, Actinobacteria, and Firmicutes. However, ECS showed an underrepresentation of Bacteroides and an enrichment of opportunistic pathogenic species of the ESKAPE group, starting from the second week. Besides revealing the intestinal microbiota of Tunisian newborns, this study provides novel insights into the microbiota perturbations caused by ECS.

Published
2022
Full Text
View/download PDF

22. The African Human Microbiome Portal: a public web portal of curated metagenomic metadata

Author

Kiran, Anmol, primary, Hanachi, Mariem, additional, Alsayed, Nihad, additional, Fassatoui, Meriem, additional, Oduaran, Ovokeraye H, additional, Allali, Imane, additional, Maslamoney, Suresh, additional, Meintjes, Ayton, additional, Zass, Lyndon, additional, Rocha, Jorge Da, additional, Kefi, Rym, additional, Benkahla, Alia, additional, Ghedira, Kais, additional, Panji, Sumir, additional, Mulder, Nicola, additional, Fadlelmola, Faisal M, additional, and Souiai, Oussema, additional

Published
2024
Full Text
View/download PDF

23. Effects of land use and cultivation histories on the distribution of soil organic carbon stocks in the area of the Northern Nile Delta in Egypt

Author

Muhammad Arshad, Khaled Mohamed Khedher, Hamdi Ayed, Abir Mouldi, Farahat S. Moghanm, Mohamed Hechemi El Ouni, Nabil Benkahla, Essaied Laatar, Muhammad Bilal, and Mohamed Abdel Zaher

Subjects
soil carbon sequestration potential, soil bulk density, carbon vertical distribution, global warming, kyoto protocol, land uses, Environmental sciences, GE1-350
Abstract

Precise knowledge of the soil organic carbon (SOC) stocks under various land uses is needed to meet the Kyoto Protocol and for the sustainability of natural resources. The purpose of the present study was to (1) gauge the depth and spatial distribution of the soil bulk density (BD), soil organic carbon (OC) stocks, and soil organic matter (OM) among the various land uses in the northern Nile Delta in Egypt; (2) estimate the soil carbon sequestration rate (CSR) under different land uses in the region; and (3) establish baseline data for SOC stocks in future studies on the dynamics of SOC. The study area was divided into ten sampling zones to represent each land use in the northern Nile Delta. Each sampling zone was further divided into four sampling sites to represent virgin lands and fish farms, and twelve sites were used to represent three crop types and four cultivation histories. The crops included clover, (Trifolium alexandrinum L.), sugar beet (Beta vulgaris L.), and rice, (Oryza sativa L.) and the years spanned were 5, 15, 30 and 50. The effects of the crop type on the SBD, SOC content, and SOC stocks were significant. In general, the SOC stocks increase as the number of years of cultivation increased. Thematic maps were produced using Geographical Information Systems (GIS) mapping. The Inverse Distance Weighted (IDW) technique in ArcGIS10.4 software revealed that the spatial pattern of the SBD, OC content, and stocks conformed to the soil analysis results. The SOC stocks of the croplands and fish farms were 1.6 and 1.5 times higher, respectively, compared to those of virgin land. Rice cropland had the lowest SBD (1.34 g cm−3) and the highest OC stocks (7.46 g C kg−1). The conversion of virgin land into croplands or fish farms actively contributed to the carbon storage rate (CSR).

Published
2020
Full Text
View/download PDF

25. High-depth African genomes inform human migration and health

Author

Choudhury, Ananyo, Aron, Shaun, Botigué, Laura R., Sengupta, Dhriti, Botha, Gerrit, Bensellak, Taoufik, Wells, Gordon, Kumuthini, Judit, Shriner, Daniel, Fakim, Yasmina J., Ghoorah, Anisah W., Dareng, Eileen, Odia, Trust, Falola, Oluwadamilare, Adebiyi, Ezekiel, Hazelhurst, Scott, Mazandu, Gaston, Nyangiri, Oscar A., Mbiyavanga, Mamana, Benkahla, Alia, Kassim, Samar K., Mulder, Nicola, Adebamowo, Sally N., Chimusa, Emile R., Muzny, Donna, Metcalf, Ginger, Gibbs, Richard A., Rotimi, Charles, Ramsay, Michèle, Adeyemo, Adebowale A., Lombard, Zané, and Hanchard, Neil A.

Published
2020
Full Text
View/download PDF

26. Deep learning regularization techniques to genomics data

Author

Harouna Soumare, Alia Benkahla, and Nabil Gmati

Subjects
Deep learning, Overfitting, Regularization techniques, Dropout, Genomics, Computer engineering. Computer hardware, TK7885-7895, Electronic computers. Computer science, QA75.5-76.95
Abstract

Deep Learning algorithms have achieved a great success in many domains where large scale datasets are used. However, training these algorithms on high dimensional data requires the adjustment of many parameters. Avoiding overfitting problem is difficult. Regularization techniques such as L1 and L2 are used to prevent the parameters of training model from being large. Another commonly used regularization method called Dropout randomly removes some hidden units during the training phase. In this work, we describe some architectures of Deep Learning algorithms, we explain optimization process for training them and attempt to establish a theoretical relationship between L2-regularization and Dropout. We experimentally compare the effect of these techniques on the learning model using genomics datasets.

Published
2021
Full Text
View/download PDF

27. Magnetohydrodynamic (MHD) Natural Convection Flow of Titanium Dioxide Nanofluid Inside 3D Cavity Containing a Hot Block: Comparative with 2D Cavity

Author

Mourad Moderres, Abdelkader Boutra, Seddik Kherroubi, Hakan F. Oztop, and Youb Khaled Benkahla

Subjects
Fluid Flow and Transfer Processes, Mechanical Engineering
Abstract

The natural convection of TiO2-Water-Nanofluid in a cubic cavity, containing a hot block under the influence of the magnetic field was studied numerically. The verticals walls are cold, the bottom wall is hot and the other walls (top, front and rear) are adiabatic. This work aims to visualize the importance of taking into account the three-dimensionality of the flow in the presence of magnetic field as well as the impact of the addition of nanoparticles on heat exchange rate evolution. The governing equations are solved using the finite volume method and the SIMPLER algorithm is used for pressure-velocity coupling. The problem was simulated at different Rayleigh numbers (103 ≤ Ra ≤ 106), Hartmann numbers (0 ≤ Ha ≤ 90) and inclination angles of the magnetic field (0 ≤ ω ≤ 135°) as well as nanoparticles volume fraction (φ = 0%, φ = 5%) with fixed Prandtl number (Pr = 7). The thermal conductivity and dynamic viscosity of the nanofluid are estimated by taking into account temperature-dependent properties, using Corcione’s correlations. Based on the cooling optimization of cold walls along with comparative analysis between 3D cavity and 2D cavity, the obtained results show that the buoyancy force enhances the heat exchange, while the magnetic field produces opposite effects. When the buoyancy force is dominated, the intensification of heat transfer becomes large, compared to the case where conduction is dominant. The qualitative difference between a 3D and 2D configuration is remarkable for higher Ra, and becomes smaller when the magnetic field is applied horizontally or vertically with relatively high intensity. But, quantitatively, the 3D flow is far from being considered as a 2D flow for all pertinent parameters control. Finally, adding nanoparticles enhances heat transfer for both configurations, the best transfer rate is obtained for ω = 0.

Published
2023

28. Epidemiological and Phylogeographic Study of Equid Herpesviruses in Tunisia

Author

Chaima Badr, Oussama Souiai, Marwa Arbi, Imen El Behi, Mohamed S. Essaied, Ines Khosrof, Alia Benkahla, Ahmed Chabchoub, and Abdeljelil Ghram

Subjects
equine, herpesvirus, EHV1, EHV2, EHV5, gB, Medicine
Abstract

Equid herpesvirus (EHV) is a contagious viral disease affecting horses, causing illness characterized by respiratory symptoms, abortion and neurological disorders. It is common worldwide and causes severe economic losses to the equine industry. The present study was aimed at investigating the incidence of EHVs, the genetic characterization of Tunisian isolates and a spatiotemporal study, using 298 collected samples from diseased and clinically healthy horses. The global incidence of EHV infection was found to be about 71.81%. EHV2 and EHV5 were detected in 146 (48.99%) and 159 (53.35%) sampled horses, respectively. EHV1 was detected in 11 samples (3.69%); EHV4 was not detected. Co-infections with EHV1-EHV2, EHV1-EHV5 and EHV2-EHV5 were observed in 0.33%, 1.34% and 31.54% of tested horses, respectively. Phylogenetic analyses showed that gB of EHV2 and EHV5 displays high genetic diversity with a nucleotide sequence identity ranging from 88 to 100% for EHV2 and 97.5 to 100% for EHV5. Phylogeography suggested Iceland and USA as the most likely countries of origin of the Tunisian EHV2 and EHV5 isolates. These viruses detected in Tunisia seemed to be introduced in the 2000s. This first epidemiological and phylogeographic study is important for better knowledge of the evolution of equid herpesvirus infections in Tunisia.

Published
2022
Full Text
View/download PDF

29. Enabling the genomic revolution in Africa

Author

Rotimi, Charles, Abayomi, Akin, Abimiku, Alash'le, Adabayeri, Victoria May, Adebamowo, Clement, Adebiyi, Ezekiel, Ademola, Adebowale D, Adeyemo, Adebowale, Adu, Dwomoa, Affolabi, Dissou, Agongo, Godfred, Ajayi, Samuel, Akarolo-Anthony, Sally, Akinyemi, Rufus, Akpalu, Albert, Alberts, Marianne, Alonso Betancourt, Orlando, Alzohairy, Ahmed Mansour, Ameni, Gobena, Amodu, Olukemi, Anabwani, Gabriel, Andersen, Kristian, Arogundade, Fatiu, Arulogun, Oyedunni, Asogun, Danny, Bakare, Rasheed, Balde, Naby, Baniecki, Mary Lynn, Beiswanger, Christine, Benkahla, Alia, Bethke, Lara, Boehnke, Micheal, Boima, Vincent, Brandful, James, Brooks, Andrew I, Brosius, Frank C, Brown, Chester, Bucheton, Bruno, Burke, David T, Burnett, Barrington G, Carrington-Lawrence, Stacy, Carstens, Nadia, Chisi, John, Christoffels, Alan, Cooper, Richard, Cordell, Heather, Crowther, Nigel, Croxton, Talishiea, de Vries, Jantina, Derr, Leslie, Donkor, Peter, Doumbia, Seydou, Duncanson, Audrey, Ekem, Ivy, El Sayed, Ahmed, Engel, Mark E, Enyaru, John CK, Everett, Dean, Fadlelmola, Faisal M, Fakunle, Eyitayo, Fischbeck, Kenneth H, Fischer, Anne, Folarin, Onikepe, Gamieldien, Junaid, Garry, Robert F, Gaseitsiwe, Simani, Gbadegesin, Rasheed, Ghansah, Anita, Giovanni, Maria, Goesbeck, Parham, Gomez-Olive, F Xavier, Grant, Donald S, Grewal, Ravnit, Guyer, Mark, Hanchard, Neil A, Happi, Christian T, Hazelhurst, Scott, Hennig, Branwen J, Hertz-, Christiane, Fowler, Hide, Winston, Hilderbrandt, Friedhelm, Hugo-Hamman, Christopher, Ibrahim, Muntaser E, James, Regina, Jaufeerally-Fakim, Yasmina, Jenkins, Carolyn, Jentsch, Ute, Jiang, Pan-Pan, Joloba, Moses, Jongeneel, Victor, Joubert, Fourie, Kader, Mukthar, Kahn, Kathleen, Kaleebu, Pontiano, Kapiga, Saidi H, Kassim, Samar Kamal, Kasvosve, Ishmael, Kayondo, Jonathan, and Keavney, Bernard

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Clinical Sciences, Medical Microbiology, Human Genome, Cancer, Infectious Diseases, HIV/AIDS, Clinical Research, Biotechnology, Rare Diseases, 2.6 Resources and infrastructure (aetiology), Aetiology, Infection, Good Health and Well Being, Africa, Disease, England, Genetics, Medical, Genome-Wide Association Study, Genomics, Health, Humans, National Institutes of Health (U.S.), United States, H3Africa Consortium, General Science & Technology
Abstract

H3Africa is developing capacity for health-related genomics research in Africa

Published
2014

30. Genome Sequence of the Tsetse Fly (Glossina morsitans): Vector of African Trypanosomiasis

Author

Initiative, International Glossina Genome, Attardo, Geoffrey M, Abila, Patrick P, Auma, Joanna E, Baumann, Aaron A, Benoit, Joshua B, Brelsfoard, Corey L, Ribeiro, José MC, Cotton, James A, Pham, Daphne QD, Darby, Alistair C, Van Den Abbeele, Jan, Denlinger, David L, Field, Linda M, Nyanjom, Steven RG, Gaunt, Michael W, Geiser, Dawn L, Gomulski, Ludvik M, Haines, Lee R, Hansen, Immo A, Jones, Jeffery W, Kibet, Caleb K, Kinyua, Johnson K, Larkin, Denis M, Lehane, Michael J, Rio, Rita VM, Macdonald, Sandy J, Macharia, Rosaline W, Malacrida, Anna R, Marco, Heather G, Marucha, Kevin K, Masiga, Daniel K, Meuti, Megan E, Mireji, Paul O, Obiero, George FO, Koekemoer, Jacobus JO, Okoro, Chinyere K, Omedo, Irene A, Osamor, Victor C, Balyeidhusa, Apollo SP, Peyton, Justin T, Price, David P, Quail, Michael A, Ramphul, Urvashi N, Rawlings, Neil D, Riehle, Michael A, Robertson, Hugh M, Sanders, Mandy J, Scott, Maxwell J, Dashti, Zahra Jalali Sefid, Snyder, Anna K, Srivastava, Tulika P, Stanley, Eleanor J, Swain, Martin T, Hughes, Daniel ST, Tarone, Aaron M, Taylor, Todd D, Telleria, Erich L, Thomas, Gavin H, Walshe, Deirdre P, Wilson, Richard K, Winzerling, Joy J, Acosta-Serrano, Alvaro, Aksoy, Serap, Arensburger, Peter, Aslett, Martin, Bateta, Rosemary, Benkahla, Alia, Berriman, Matthew, Bourtzis, Kostas, Caers, Jelle, Caljon, Guy, Christoffels, Alan, Falchetto, Marco, Friedrich, Markus, Fu, Shuhua, Gäde, Gerd, Githinji, George, Gregory, Richard, Hall, Neil, Harkins, Gordon, Hattori, Masahira, Hertz-Fowler, Christiane, Hide, Winston, Hu, Wanqi, Imanishi, Tadashi, Inoue, Noboru, Jonas, Mario, Kawahara, Yoshihiro, Koffi, Mathurin, Kruger, Adele, Lawson, Daniel, Lehane, Stella, Lehväslaiho, Heikki, Luiz, Thiago, Makgamathe, Mmule, Malele, Imna, Manangwa, Oliver, Manga, Lucien, and Megy, Karyn

Subjects
Vector-Borne Diseases, Genetics, Prevention, Infectious Diseases, Biotechnology, 2.2 Factors relating to the physical environment, Aetiology, Infection, Good Health and Well Being, Animals, Blood, Feeding Behavior, Female, Genes, Insect, Genome, Insect, Insect Proteins, Insect Vectors, Microbiota, Molecular Sequence Annotation, Molecular Sequence Data, Reproduction, Salivary Glands, Sensation, Sequence Analysis, DNA, Symbiosis, Trypanosoma, Trypanosomiasis, African, Tsetse Flies, Wolbachia, International Glossina Genome Initiative, General Science & Technology
Abstract

Tsetse flies are the sole vectors of human African trypanosomiasis throughout sub-Saharan Africa. Both sexes of adult tsetse feed exclusively on blood and contribute to disease transmission. Notable differences between tsetse and other disease vectors include obligate microbial symbioses, viviparous reproduction, and lactation. Here, we describe the sequence and annotation of the 366-megabase Glossina morsitans morsitans genome. Analysis of the genome and the 12,308 predicted protein-encoding genes led to multiple discoveries, including chromosomal integrations of bacterial (Wolbachia) genome sequences, a family of lactation-specific proteins, reduced complement of host pathogen recognition proteins, and reduced olfaction/chemosensory associated genes. These genome data provide a foundation for research into trypanosomiasis prevention and yield important insights with broad implications for multiple aspects of tsetse biology.

Published
2014

31. Developing Clinical Phenotype Data Collection Standards for Research in Africa

Author

Zass, Lyndon, primary, Johnston, Katherine, additional, Benkahla, Alia, additional, Chaouch, Melek, additional, Kumuthini, Judit, additional, Radouani, Fouzia, additional, Mwita, Liberata Alexander, additional, Alsayed, Nihad, additional, Allie, Taryn, additional, Sathan, Dassen, additional, Masamu, Upendo, additional, Seuneu Tchamga, Milaine Sergine, additional, Tamuhla, Tsaone, additional, Samtal, Chaimae, additional, Nembaware, Victoria, additional, Gill, Zoe, additional, Ahmed, Samah, additional, Hamdi, Yosr, additional, Fadlelmola, Faisal, additional, Tiffin, Nicki, additional, and Mulder, Nicola, additional

Published
2023
Full Text
View/download PDF

32. Cancer in Africa: The Untold Story

Author

Yosr Hamdi, Ines Abdeljaoued-Tej, Afzal Ali Zatchi, Sonia Abdelhak, Samir Boubaker, Joel S. Brown, and Alia Benkahla

Subjects
cancer, Africa, epidemiology, incidence rates, mortality rates, risk factors, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

BackgroundDespite rising incidence and mortality rates in Africa, cancer has been given low priority in the research field and in healthcare services. Indeed, 57% of all new cancer cases around the world occur in low income countries exacerbated by lack of awareness, lack of preventive strategies, and increased life expectancies. Despite recent efforts devoted to cancer epidemiology, statistics on cancer rates in Africa are often dispersed across different registries. In this study our goal included identifying the most promising prevention and treatment approaches available in Africa. To do this, we collated and analyzed the incidence and fatality rates for the 10 most common and fatal cancers in 56 African countries grouped into 5 different regions (North, West, East, Central and South) over 16-years (2002–2018). We examined temporal and regional trends by investigating the most important risk factors associated to each cancer type. Data were analyzed by cancer type, African region, gender, measures of socioeconomic status and the availability of medical devices.ResultsWe observed that Northern and Southern Africa were most similar in their cancer incidences and fatality rates compared to other African regions. The most prevalent cancers are breast, bladder and liver cancers in Northern Africa; prostate, lung and colorectal cancers in Southern Africa; and esophageal and cervical cancer in East Africa. In Southern Africa, fatality rates from prostate cancer and cervical cancer have increased. In addition, these three cancers are less fatal in Northern and Southern Africa compared to other regions, which correlates with the Human Development Index and the availability of medical devices. With the exception of thyroid cancer, all other cancers have higher incidences in males than females.ConclusionOur results show that the African continent suffers from a shortage of medical equipment, research resources and epidemiological expertise. While recognizing that risk factors are interconnected, we focused on risk factors more or less specific to each cancer type. This helps identify specific preventive and therapeutic options in Africa. We see a need for implementing more accurate preventive strategies to tackle this disease as many cases are likely preventable. Opportunities exist for vaccination programs for cervical and liver cancer, genetic testing and use of new targeted therapies for breast and prostate cancer, and positive changes in lifestyle for lung, colorectal and bladder cancers. Such recommendations should be tailored for the different African regions depending on their disease profiles and specific needs.

Published
2021
Full Text
View/download PDF

38. Vemurafenib Inhibits Acute and Chronic Enterovirus Infection by Affecting Cellular Kinase Phosphatidylinositol 4-Kinase Type IIIβ

Author

Laajala, Mira, primary, Zwaagstra, Marleen, additional, Martikainen, Mari, additional, Nekoua, Magloire Pandoua, additional, Benkahla, Mehdi, additional, Sane, Famara, additional, Gervais, Emily, additional, Campagnola, Grace, additional, Honkimaa, Anni, additional, Sioofy-Khojine, Amir-Babak, additional, Hyöty, Heikki, additional, Ojha, Ravi, additional, Bailliot, Marie, additional, Balistreri, Giuseppe, additional, Peersen, Olve, additional, Hober, Didier, additional, Van Kuppeveld, Frank, additional, and Marjomäki, Varpu, additional

Published
2023
Full Text
View/download PDF

41. Vemurafenib Inhibits Acute and Chronic Enterovirus Infection by Affecting Cellular Kinase Phosphatidylinositol 4-Kinase Type IIIb

Author

Laajala, Mira, Zwaagstra, Marleen, Martikainen, Mari, Nekoua, Magloire Pandoua, Benkahla, Mehdi, Sane, Famara, Gervais, Emily, Campagnola, Grace, Honkimaa, Anni, Sioofy-Khojine, Amir-Babak, Hyöty, Heikki, Ojha, Ravi, Bailliot, Marie, Balistreri, Giuseppe, Peersen, Olve, Hober, Didier, Van Kuppeveld, Frank, Marjomäki, Varpu, Laajala, Mira, Zwaagstra, Marleen, Martikainen, Mari, Nekoua, Magloire Pandoua, Benkahla, Mehdi, Sane, Famara, Gervais, Emily, Campagnola, Grace, Honkimaa, Anni, Sioofy-Khojine, Amir-Babak, Hyöty, Heikki, Ojha, Ravi, Bailliot, Marie, Balistreri, Giuseppe, Peersen, Olve, Hober, Didier, Van Kuppeveld, Frank, and Marjomäki, Varpu

Abstract

Enteroviruses are one of the most abundant viruses causing mild to serious acute infections in humans and also contributing to chronic diseases like type 1 diabetes. Presently, there are no approved antiviral drugs against enteroviruses. Here, we studied the potency of vemurafenib, an FDA-Approved RAF kinase inhibitor for treating BRAFV600E mutant-related melanoma, as an antiviral against enteroviruses. We showed that vemurafenib prevented enterovirus translation and replication at low micromolar dosage in an RAF/MEK/ERK-independent manner. Vemurafenib was effective against group A, B, and C enteroviruses, as well as rhinovirus, but not parechovirus or more remote viruses such as Semliki Forest virus, adenovirus, and respiratory syncytial virus. The inhibitory effect was related to a cellular phosphatidylinositol 4-kinase type IIIb (PI4KB), which has been shown to be important in the formation of enteroviral replication organelles. Vemurafenib prevented infection efficiently in acute cell models, eradicated infection in a chronic cell model, and lowered virus amounts in pancreas and heart in an acute mouse model. Altogether, instead of acting through the RAF/MEK/ERK pathway, vemurafenib affects the cellular PI4KB and, hence, enterovirus replication, opening new possibilities to evaluate further the potential of vemurafenib as a repurposed drug in clinical care. IMPORTANCE Despite the prevalence and medical threat of enteroviruses, presently, there are no antivirals against them. Here, we show that vemurafenib, an FDA-Approved RAF kinase inhibitor for treating BRAFV600E mutant-related melanoma, prevents enterovirus translation and replication. Vemurafenib shows efficacy against group A, B, and C enteroviruses, as well as rhinovirus, but not parechovirus or more remote viruses such as Semliki Forest virus, adenovirus, and respiratory syncytial virus. The inhibitory effect acts through cellular phosphatidylinositol 4-kinase type IIIb (PI4KB), which has been shown to

Published
2023

42. Vemurafenib Inhibits Acute and Chronic Enterovirus Infection by Affecting Cellular Kinase Phosphatidylinositol 4-Kinase Type IIIb

Author

Virologie, Infectious Diseases and Immunology - Virology, Laajala, Mira, Zwaagstra, Marleen, Martikainen, Mari, Nekoua, Magloire Pandoua, Benkahla, Mehdi, Sane, Famara, Gervais, Emily, Campagnola, Grace, Honkimaa, Anni, Sioofy-Khojine, Amir-Babak, Hyöty, Heikki, Ojha, Ravi, Bailliot, Marie, Balistreri, Giuseppe, Peersen, Olve, Hober, Didier, Van Kuppeveld, Frank, Marjomäki, Varpu, Virologie, Infectious Diseases and Immunology - Virology, Laajala, Mira, Zwaagstra, Marleen, Martikainen, Mari, Nekoua, Magloire Pandoua, Benkahla, Mehdi, Sane, Famara, Gervais, Emily, Campagnola, Grace, Honkimaa, Anni, Sioofy-Khojine, Amir-Babak, Hyöty, Heikki, Ojha, Ravi, Bailliot, Marie, Balistreri, Giuseppe, Peersen, Olve, Hober, Didier, Van Kuppeveld, Frank, and Marjomäki, Varpu

Published
2023

44. Retrospective Phylodynamic and Phylogeographic Analysis of the Bluetongue Virus in Tunisia.

Author

Souiai, Oussema, Arbi, Marwa, Hanachi, Mariem, Sallami, Ameny, Larbi, Imen, Chaouch, Melek, Harigua-Souiai, Emna, and Benkahla, Alia

Subjects
BLUETONGUE virus, ARBOVIRUSES, VIRAL transmission, PHYLOGEOGRAPHY, SEROTYPES, RICE blast disease, POTATO virus Y
Abstract

Bluetongue virus (BTV) is an arbovirus considered as a major threat for the global livestock economy. Since 1999, Tunisia has experienced several incursions of BTV, during which numerous cases of infection and mortality have been reported. However, the geographical origin and epidemiological characteristics of these incursions remained unclear. To understand the evolutionary history of BTV emergence in Tunisia, we extracted from Genbank the segment 6 sequences of 7 BTV strains isolated in Tunisia during the period 2000 to 2017 and blasted them to obtain a final dataset of 67 sequences. We subjected the dataset to a Bayesian phylogeography framework inferring geographical origin and serotype as phylodynamic models. Our results suggest that BTV-2 was first introduced in Tunisia in the 1960s and that since 1990s, the country has witnessed the emergence of other typical and atypical BTV serotypes notably BTV-1, BTV-3 and BTV-Y. The reported serotypes have a diverse geographical origin and have been transmitted to Tunisia from countries in the Mediterranean Basin. Interserotype reassortments have been identified among BTV-1, BTV-2 and BTV-Y. This study has provided new insights on the temporal and geographical origin of BTV in Tunisia, suggesting the contribution of animal trade and environment conditions in virus spread. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

45. Upregulation of HLA class II in pancreatic beta cells from organ donors with type 1 diabetes

Author

Estefania Quesada-Masachs, Samuel Zilberman, Sakthi Rajendran, Tiffany Chu, Sara McArdle, William B. Kiosses, Jae-Hyun M. Lee, Burcak Yesildag, Mehdi A. Benkahla, Agnieszka Pawlowska, Madeleine Graef, Susanne Pfeiffer, Zbigniew Mikulski, and Matthias von Herrath

Subjects
Adult, Male, Adolescent, Endocrinology, Diabetes and Metabolism, Histocompatibility Antigens Class II, Tissue Donors, Up-Regulation, Young Adult, Diabetes Mellitus, Type 1, Glucose, Insulin-Secreting Cells, Insulin Secretion, Internal Medicine, Humans, Insulin, Female, Child, Cells, Cultured, Autoantibodies
Abstract

We aimed to characterise and quantify the expression of HLA class II (HLA-II) in human pancreatic tissue sections and to analyse its induction in human islets.We immunostained human pancreatic tissue sections from non-diabetic (n = 5), autoantibody positive (Aab+; n = 5), and type 1 diabetic (n = 5) donors, obtained from the Network of Pancreatic Organ Donors (nPOD), with HLA-II, CD68 and insulin. Each tissue section was acquired with a widefield slide scanner and then analysed with QuPath software. In total, we analysed 7415 islets that contained 338,480 cells. Widefield microscopy was further complemented by high resolution imaging of 301 randomly selected islets, acquired using a Zeiss laser scanning confocal (LSM880) to confirm our findings. Selected beta cells were acquired in enhanced resolution using LSM880 with an Airyscan detector. Further, we cultured healthy isolated human islets and reaggregated human islet microtissues with varying concentrations of proinflammatory cytokines (IFN-γ, TNF-α and IL-1β). After proinflammatory cytokine culture, islet function was measured by glucose-stimulated insulin secretion, and HLA-I and HLA-II expression was subsequently evaluated with immunostaining or RNA sequencing.Insulin-containing islets (ICIs) of donors with type 1 diabetes had a higher percentage of HLA-II positive area (24.31%) compared with type 1 diabetic insulin-deficient islets (IDIs, 0.67%), non-diabetic (3.80%), and Aab+ (2.31%) donors. In ICIs of type 1 diabetic donors, 45.89% of the total insulin signal co-localised with HLA-II, and 27.65% of the islet beta cells expressed both HLA-II and insulin, while in non-diabetic and Aab+ donors 0.96% and 0.59% of the islet beta cells, respectively, expressed both markers. In the beta cells of donors with type 1 diabetes, HLA-II was mostly present in the cell cytoplasm, co-localising with insulin. In the experiments with human isolated islets and reaggregated human islets, we observed changes in insulin secretion upon stimulation with proinflammatory cytokines, as well as higher expression of HLA-II and HLA-I when compared with controls cultured with media, and an upregulation of HLA-I and HLA-II RNA transcripts.After a long-standing controversy, we provide definitive evidence that HLA-II can be expressed by pancreatic beta cells from patients with type 1 diabetes. Furthermore, this upregulation can be induced in vitro in healthy isolated human islets or reaggregated human islets by treatment with proinflammatory cytokines. Our findings support a role for HLA-II in type 1 diabetes pathogenesis since HLA-II expressing beta cells can potentially become a direct target of autoreactive CD4

Published
2021

46. Entropy generation due to the mixed convection flow of MWCNT−MgO/water hybrid nanofluid in a vented complex shape cavity

Author

Benzema Mahdi, Benkahla Youb Khaled, Boudiaf Ahlem, Ouyahia Seif-Eddine, and El Ganaoui Mohammed

Subjects
Engineering (General). Civil engineering (General), TA1-2040
Abstract

This paper reports a numerical study of mixed convection heat transfer with entropy generation in a vented complex shape cavity filled with MWCNT−MgO (15:85 vol %) /water hybrid nanofluid. A hot source is placed at the mid potion of the inclined plate of the enclosure, while the rest of the rigid walls are adiabatic. A thermo-dependent correlations proposed by [12] for the dynamic viscosity and the thermal conductivity, especially developed for the considered fluid, are used. After validation of the model, the analysis has been done for a Reynolds numbers ranging from 10 to 600 and total nanoparticles volume fraction ranging from 0.0 to 0.02 using the finite volume method. The predicted results of streamlines, isotherms, isentropic lines, average Nusselt number, average entropy generation and average Bejan number are the main focus of interest in the present paper.

Published
2020
Full Text
View/download PDF

47. Heat transfer analysis of nanofluid flow through backward facing step

Author

Boudiaf Ahlem, Danane Fetta, Benkahla Youb Khaled, Berabou Walid, Benzema Mahdi, and Ouyahia Seif-Eddine

Subjects
Engineering (General). Civil engineering (General), TA1-2040
Abstract

This paper presents the numerical predictions of hydrodynamic and thermal characteristics of nanofluid flow through backward facing step. The governing equations are solved through the finite volume method, as described by Patankar, by taking into account the associated boundary conditions. Empirical relations were used to give the effective dynamic viscosity and the thermal conductivity of the nanofluid. Effects of different key parameters such as Reynolds number, nanoparticle solid volume fraction and nanoparticle solid diameter on the heat transfer and fluid flow are investigated. The results are discussed in terms of the average Nusselt number and streamlines.

Published
2020
Full Text
View/download PDF

48. Heat transfer and fluid flow of Biodiesel at a backward-Facing step

Author

Danane Fetta, Bessah Rahma, Mahfoud Omar, Boudiaf Ahlem, Ahmia Aida.Cherifa, Ouyahia Seif-Eddine, Alloune Rhiad, and Benkahla Youb.Khaled

Subjects
Engineering (General). Civil engineering (General), TA1-2040
Abstract

You should Three-dimensional simulation of a biodiesel fluid flow within a rectangular duct over a backward-facing step is investigated in the present paper. The fluid, which obeys to the Newtonian rheological behavior, is obtained by transformation of Algerian waste cooking oil into a biodiesel. Flow through a rectangular channel subjected to a constant wall temperature or constant heat flux as boundary conditions. The partial differential equations governing fluid flow and heat transfer are solved by the Fluent CFD computational code based on the Finite Volume Method. The numerical experiments are carried out to examine the effect of the Reynolds number by fluid inlet velocity variation for the two boundary conditions. The results are analyzed through the distribution of the temperature and the velocity contours. The variation of the Reynolds number and boundary conditions affects greatly the heat transfer and the fluid flow, in particular near the step region.

Published
2020
Full Text
View/download PDF

49. Numerical Study of Heat and Mass Transfer during the Evaporative Drying of Porous Media

Author

SELLAMI Karima, FEDDAOUI M’barek, LABSI Nabila, OUBELLA M’hand, and BENKAHLA Youb Khaled

Subjects
drying, evaporation, wet porous layer, finite volume methods, Engineering (General). Civil engineering (General), TA1-2040
Abstract

The paper deals with numerical study of drying process of porous media of sand during the evaporation of a liquid saturated porous layer within parallel vertical channel. The liquid and air streams are modeled as two coupled laminar boundary layers incorporating non-Darcian models of the inertia and boundary effects. The governing equations and the associated boundary conditions are discretized by means of the finite volume method implemented on a staggered mesh and the velocity-pressure coupling is processed by the SIMPLER algorithm. The influences of the inlet mass flow of the drying gas, porous layer thickness and the porosity on the drying process are analyzed. Results show that the drying rate of the porous media is improved by the reduction of the porosity and porous layer thickness a large drying rate is obtained with high inlet mass flow and high inlet gas temperature.

Published
2020
Full Text
View/download PDF

50. Simulation of Natural Convection in a horizontal channel with heat sources mounted with porous blocks by the lattice Boltzmann method (MRT-LBM)

Author

BOUARNOUNA Kaoutar, BOUTRA Abdelkader, BENZEMA Mahdi, El Ganaoui Mohammed, and BENKAHLA Youb Khaled

Subjects
Engineering (General). Civil engineering (General), TA1-2040
Abstract

In this paper, laminar natural convection in a horizontal channel provided with porous blocks periodically distributed on its lower adiabatic surface has been analyzed. This numerical study is based on the multiple-relaxation-time (MRT) Lattice Boltzmann method (LBM). The two-dimensional model D2Q9 is adopted to solve the flow field, while the D2Q5 model is applied to solve the temperature field. The objective of the study is to analyze the effect of the Darcy number (10-1 ≤ Da ≤ 10-6), Rayleigh number (103 ≤ Ra ≤ 107) and the relative porous blocks height (1/8 ≤ D ≤ 1/2). The obtained results show the important effect of these parameters, which cannot be neglected, on both flow and the heat transfer structure, within this kind of channels.

Published
2020
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results