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2. Global cross-cultural validation of a brief measure for identifying potential suicide risk in 42 countries

Author

Gewirtz-Meydan, A., Koós, M., Nagy, L., Kraus, S.W., Demetrovics, Z., Potenza, M.N., Ballester-Arnal, R., Batthyány, D., Bergeron, S., Billieux, J., Burkauskas, J., Cárdenas-López, G., Carvalho, J., Castro-Calvo, J., Chen, L., Ciocca, G., Corazza, O., Csako, R., Fernandez, D.P., Fujiwara, H., Fernandez, E.F., Fuss, J., Gabrhelík, R., Gjoneska, B., Gola, M., Grubbs, J.B., Hashim, H.T., Islam, M.S., Ismail, M., Jiménez-Martínez, M.C., Jurin, T., Kalina, O., Klein, V., Költő, A., Lee, S.-K., Lewczuk, K., Lin, C.-Y., Lochner, C., López-Alvarado, S., Lukavská, K., Mayta-Tristán, P., Miller, D.J., Orosová, O., Orosz, G., Ponce, F.P., Quintana, G.R., Quintero Garzola, G.C., Ramos-Diaz, J., Rigaud, K., Rousseau, A., De Tubino Scanavino, M., Schulmeyer, M.K., Sharan, P., Shibata, M., Shoib, S., Sigre-Leirós, V., Sniewski, L., Spasovski, O., Steibliene, V., Stein, D.J., Strong, C., Ünsal, B.C., Vaillancourt-Morel, M.-P., Van Hout, M.C., and Bőthe, B.

Published
2024
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4. Analysis of SIGLEC12 expression, immunomodulation and prognostic value in renal cancer using multiomic databases

Author

Amobichukwu K. Ogbodo, Denis Mustafov, Mohit Arora, George I. Lambrou, Maria Braoudaki, and Shoib S. Siddiqui

Subjects
SIGLEC12, Immunotherapy, Carcinomas, Kidney, KM plotter, UALCAN, Science (General), Q1-390, Social sciences (General), H1-99
Abstract

Siglecs belong to a family of immune regulatory receptors predominantly found on hematopoietic cells. They interact with Sia, resulting in the activation or inhibition of the immune response. Previous reports have suggested that the SIGLEC12 gene, which encodes the Siglec-XII protein, is expressed in the epithelial tissues and upregulated in carcinomas. However, studies deciphering the role of Siglec-XII in renal cancer (RC) are still unavailable, and here we provide insights on this question. We conducted expression analysis using the Human Protein Atlas and UALCAN databases. The impact of SIGLEC12 on RC prognosis was determined using the KM plotter, and an assessment of immune infiltration with SIGLEC12 was performed using the TIMER database. GSEA was conducted to identify the pathways affected by SIGLEC12. Finally, using GeneMania, we identified Siglec-XII interacting proteins. Our findings indicated that macrophages express SIGLEC12 in the kidney. Furthermore, we hypothesize that Siglec-XII expression might be involved in the increase of primary RC, but this effect may not be dependent on the age of the patient. In the tumour microenvironment, oncogenic pathways appeared to be upregulated by SIGLEC12. Similarly, our analysis suggested that SIGLEC12-related kidney renal papillary cell carcinomas may be more suitable for targeted immunotherapy, such as CTLA-4 and PD-1/PD-L1 inhibitors. These preliminary results suggested that high expression of SIGLEC12 is associated with poor prognosis for RC. Future studies to assess its clinical utility are necessitated.

Published
2024
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5. Sialoglycan recognition is a common connection linking acidosis, zinc, and HMGB1 in sepsis

Author

Siddiqui, Shoib S, Dhar, Chirag, Sundaramurthy, Venkatasubramaniam, Sasmal, Aniruddha, Yu, Hai, Bandala-Sanchez, Esther, Li, Miaomiao, Zhang, Xiaoxiao, Chen, Xi, Harrison, Leonard C, Xu, Ding, and Varki, Ajit

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Sepsis, Infectious Diseases, Hematology, Inflammatory and immune system, Acidosis, Carrier Proteins, HMGB1 Protein, Humans, Hydrogen-Ion Concentration, Immunity, Innate, Lipopolysaccharides, Polysaccharides, Sialic Acids, Sialoglycoproteins, Zinc, sialic acid, Neu5Ac, COVID-19, cytokine storm, HMGB1
Abstract

Blood pH is tightly maintained between 7.35 and 7.45, and acidosis (pH

Published
2021

6. Evolutionary conservation of human ketodeoxynonulosonic acid production is independent of sialoglycan biosynthesis

Author

Kawanishi, Kunio, Saha, Sudeshna, Diaz, Sandra, Vaill, Michael, Sasmal, Aniruddha, Siddiqui, Shoib S, Choudhury, Biswa P, Sharma, Kumar, Chen, Xi, Schoenhofen, Ian C, Sato, Chihiro, Kitajima, Ken, Freeze, Hudson H, Münster-Kühnel, Anja, and Varki, Ajit

Subjects
2.1 Biological and endogenous factors, Aetiology, Atherosclerosis, HEK293 Cells, Human Umbilical Vein Endothelial Cells, Humans, Kidney Failure, Chronic, N-Acetylneuraminic Acid, Polysaccharides, Glycobiology, Metabolism, Nephrology, Medical and Health Sciences, Immunology
Abstract

Human metabolic incorporation of nonhuman sialic acid (Sia) N-glycolylneuraminic acid into endogenous glycans generates inflammation via preexisting antibodies, which likely contributes to red meat-induced atherosclerosis acceleration. Exploring whether this mechanism affects atherosclerosis in end-stage renal disease (ESRD), we instead found serum accumulation of 2-keto-3-deoxy-d-glycero-d-galacto-2-nonulosonic acid (Kdn), a Sia prominently expressed in cold-blooded vertebrates. In patients with ESRD, levels of the Kdn precursor mannose also increased, but within a normal range. Mannose ingestion by healthy volunteers raised the levels of urinary mannose and Kdn. Kdn production pathways remained conserved in mammals but were diminished by an M42T substitution in a key biosynthetic enzyme, N-acetylneuraminate synthase. Remarkably, reversion to the ancestral methionine then occurred independently in 2 lineages, including humans. However, mammalian glycan databases contain no Kdn-glycans. We hypothesize that the potential toxicity of excess mannose in mammals is partly buffered by conversion to free Kdn. Thus, mammals probably conserve Kdn biosynthesis and modulate it in a lineage-specific manner, not for glycosylation, but to control physiological mannose intermediates and metabolites. However, human cells can be forced to express Kdn-glycans via genetic mutations enhancing Kdn utilization, or by transfection with fish enzymes producing cytidine monophosphate-Kdn (CMP-Kdn). Antibodies against Kdn-glycans occur in pooled human immunoglobulins. Pathological conditions that elevate Kdn levels could therefore result in antibody-mediated inflammatory pathologies.

Published
2021

7. Human‐specific polymorphic pseudogenization of SIGLEC12 protects against advanced cancer progression

Author

Siddiqui, Shoib S, Vaill, Michael, Do, Raymond, Khan, Naazneen, Verhagen, Andrea L, Zhang, Wu, Lenz, Heinz‐Josef, Johnson‐Pais, Teresa L, Leach, Robin J, Fraser, Gary, Wang, Charles, Feng, Gen‐Sheng, Varki, Nissi, and Varki, Ajit

Subjects
Biological Sciences, Genetics, Biotechnology, Human Genome, Urologic Diseases, Cancer, 2.1 Biological and endogenous factors, advanced carcinoma, dot blot, immunohistochemistry, pseudogenization, SIGLEC12, Biological sciences
Abstract

Compared with our closest living evolutionary cousins, humans appear unusually prone to develop carcinomas (cancers arising from epithelia). The SIGLEC12 gene, which encodes the Siglec-XII protein expressed on epithelial cells, has several uniquely human features: a fixed homozygous missense mutation inactivating its natural ligand recognition property; a polymorphic frameshift mutation eliminating full-length protein expression in ~60%-70% of worldwide human populations; and, genomic features suggesting a negative selective sweep favoring the pseudogene state. Despite the loss of canonical sialic acid binding, Siglec-XII still recruits Shp2 and accelerates tumor growth in a mouse model. We hypothesized that dysfunctional Siglec-XII facilitates human carcinoma progression, correlating with known tumorigenic signatures of Shp2-dependent cancers. Immunohistochemistry was used to detect Siglec-XII expression on tissue microarrays. PC-3 prostate cancer cells were transfected with Siglec-XII and transcription of genes enriched with Siglec-XII was determined. Genomic SIGLEC12 status was determined for four different cancer cohorts. Finally, a dot blot analysis of human urinary epithelial cells was established to determine the Siglec-XII expressors versus non-expressors. Forced expression in a SIGLEC12 null carcinoma cell line enriched transcription of genes associated with cancer progression. While Siglec-XII was detected as expected in ~30%-40% of normal epithelia, ~80% of advanced carcinomas showed strong expression. Notably, >80% of late-stage colorectal cancers had a functional SIGLEC12 allele, correlating with overall increased mortality. Thus, advanced carcinomas are much more likely to occur in individuals whose genomes have an intact SIGLEC12 gene, likely because the encoded Siglec-XII protein recruits Shp2-related oncogenic pathways. The finding has prognostic, diagnostic, and therapeutic implications.

Published
2021

8. Dual actions of group B Streptococcus capsular sialic acid provide resistance to platelet-mediated antimicrobial killing

Author

Uchiyama, Satoshi, Sun, Josh, Fukahori, Kyoko, Ando, Nao, Wu, Mengyou, Schwarz, Flavio, Siddiqui, Shoib S, Varki, Ajit, Marth, Jamey D, and Nizet, Victor

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Biological Sciences, Prevention, Infectious Diseases, Emerging Infectious Diseases, Clinical Research, Hematology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Infection, Adult, Animals, Antigens, CD, Antigens, Differentiation, B-Lymphocyte, Bacterial Capsules, Blood Bactericidal Activity, Blood Platelets, Female, Glycocalyx, Humans, Male, Mice, Mice, Knockout, N-Acetylneuraminic Acid, Platelet Activation, Sialic Acid Binding Immunoglobulin-like Lectins, Streptococcal Infections, Streptococcus agalactiae, Virulence Factors, platelets, group B Streptococcus, innate immunity, sialic acid, Siglec
Abstract

Circulating platelets have important functions in thrombosis and in modulating immune and inflammatory responses. However, the role of platelets in innate immunity to bacterial infection is largely unexplored. While human platelets rapidly kill Staphylococcus aureus, we found the neonatal pathogen group B Streptococcus (GBS) to be remarkably resistant to platelet killing. GBS possesses a capsule polysaccharide (CPS) with terminal α2,3-linked sialic acid (Sia) residues that mimic a common epitope present on the human cell surface glycocalyx. A GBS mutant deficient in CPS Sia was more efficiently killed by human platelets, thrombin-activated platelet releasate, and synthetic platelet-associated antimicrobial peptides. GBS Sia is known to bind inhibitory Sia-recognizing Ig superfamily lectins (Siglecs) to block neutrophil and macrophage activation. We show that human platelets also express high levels of inhibitory Siglec-9 on their surface, and that GBS can engage this receptor in a Sia-dependent manner to suppress platelet activation. In a mouse i.v. infection model, antibody-mediated platelet depletion increased susceptibility to platelet-sensitive S. aureus but did not alter susceptibility to platelet-resistant GBS. Elimination of murine inhibitory Siglec-E partially reversed platelet suppression in response to GBS infection. We conclude that GBS Sia has dual roles in counteracting platelet antimicrobial immunity: conferring intrinsic resistance to platelet-derived antimicrobial components and inhibiting platelet activation through engagement of inhibitory Siglecs. We report a bacterial virulence factor for evasion of platelet-mediated innate immunity.

Published
2019

9. Motors of COVID-19 Vaccination Acceptance Scale (MoVac-COVID19S): Evidence of Measurement Invariance Across Five Countries

Author

Chen IH, Wu PL, Yen CF, Ullah I, Shoib S, Zahid SU, Bashir A, Iqbal N, Addo FM, Adjaottor ES, Amankwaah GB, Ahorsu DK, Griffiths MD, Lin CY, and Pakpour AH

Subjects
factor structure, vaccine hesitancy, young adults, Public aspects of medicine, RA1-1270
Abstract

I-Hua Chen,1,* Pei-Ling Wu,2,3,* Cheng-Fang Yen,4– 6,* Irfan Ullah,7 Sheikh Shoib,8 Shafi Ullah Zahid,9 Aadil Bashir,10 Naved Iqbal,11 Frimpong-Manso Addo,12 Emma Sethina Adjaottor,12 Gifty Boakye Amankwaah,12 Daniel Kwasi Ahorsu,13 Mark D Griffiths,14 Chung-Ying Lin,15– 18 Amir H Pakpour19 1Chinese Academy of Education Big Data, Qufu Normal University, Qufu City, Shandong, People’s Republic of China; 2School of Medicine, College of Medicine, I-Shou University, Kaohsiung, Taiwan; 3Department of Pediatrics, E-Da Hospital, Kaohsiung, Taiwan; 4Department of Psychiatry, College of Medicine, Kaohsiung Medical University, Kaohsiung, 80708, Taiwan; 5Department of Psychiatry, Kaohsiung Medical University Hospital, Kaohsiung, 80756, Taiwan; 6College of Professional Studies, National Pingtung University of Science and Technology, Pingtung, 91201, Taiwan; 7Kabir Medical College, Gandhara University, Peshawar, Pakistan; 8Sheikh Shoib Department of Psychiatry, Jawahar Lal Nehru Memorial Hospital, Srinagar, India; 9Department of Neurosurgery, Jamhuriat hospital, Kabul, Afghanistan; 10Department of Social Work, University of Kashmir, Kashmir, India; 11Department of Psychology, Jamia Millia Islamia, New Delhi, India; 12Department of Behavioural Sciences, Kwame Nkrumah University of Science and Technology, Kumasi, Ghana; 13Department of Rehabilitation Sciences, The Hong Kong Polytechnic University, Hung Hom, Hong Kong; 14International Gaming Research Unit, Psychology Department, Nottingham Trent University, Nottingham, UK; 15Institute of Allied Health Sciences, College of Medicine, National Cheng Kung University, Tainan, Taiwan; 16Biostatistics Consulting Center, National Cheng Kung University Hospital, College of Medicine, National Cheng Kung University, Tainan, Taiwan; 17Department of Occupational Therapy, College of Medicine, National Cheng Kung University, Tainan, Taiwan; 18Department of Public Health, College of Medicine, National Cheng Kung University, Tainan, Taiwan; 19Department of Nursing, School of Health and Welfare, Jönköping University, Jönköping, Sweden*These authors contributed equally to this workCorrespondence: Emma Sethina Adjaottor; Chung-Ying Lin, Tel +233 20 816 85080 ; +886-6-2353535-5106, Fax + 886-6-2367981, Email eadjaottor.chs@knust.edu.gh; cylin36933@gmail.comPurpose: The percentage of individuals who were fully vaccinated against COVID-19 was 53% worldwide, 62% in Asia, and 11% in Africa at the time of writing (February 9, 2022). In addition to administrative issues, vaccine hesitancy is an important factor contributing to the relatively low rate of vaccination. The Motors of COVID-19 Vaccination Acceptance Scale (MoVac-COVID19S) was developed to assess COVID-19 vaccination acceptance levels. However, it has only been tested among Taiwanese, mainland Chinese, and Ghanaian populations (Chen et al, 2021; Fan et al, 2021; Yeh et al, 2021). Therefore, the present study examined the construct validity and measurement invariance of the MoVac-COVID19S among individuals from five countries (ie, Taiwan, mainland China, India, Ghana, and Afghanistan).Participants and Methods: A cross-sectional survey study recruited 6053 participants across five countries who completed the survey between January and March 2021. Confirmatory factor analysis (CFA) fit indices were used to examine factor structure and measurement invariance across the five countries.Results: The fit indices of the CFA were relatively good across the countries except for the root mean square error of approximation (RMSEA). Moreover, the four-factor structure (either nine or 12 items) had a better fit than the one-factor structure. However, the four-factor model using nine MoVac-COVID19S items was the only model that had measurement invariance support for both factor loadings and item intercepts across the five countries.Conclusion: The present study confirmed that the MoVac-COVID19S has acceptable psychometric properties and can be used to assess an individual’s willingness to get COVID-19 vaccination.Keywords: factor structure, vaccine hesitancy, young adults

Published
2022

10. The Alzheimer's disease–protective CD33 splice variant mediates adaptive loss of function via diversion to an intracellular pool

Author

Siddiqui, Shoib S, Springer, Stevan A, Verhagen, Andrea, Sundaramurthy, Venkatasubramaniam, Alisson-Silva, Frederico, Jiang, Weiping, Ghosh, Pradipta, and Varki, Ajit

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Brain Disorders, Neurosciences, Alzheimer's Disease, Acquired Cognitive Impairment, Aging, Neurodegenerative, Dementia, Underpinning research, 1.1 Normal biological development and functioning, Aetiology, 2.1 Biological and endogenous factors, Neurological, Alleles, Alzheimer Disease, Amino Acid Motifs, Bacterial Proteins, Cell Line, Cell Membrane, Genetic Predisposition to Disease, Humans, Lipopolysaccharides, Macrophage Activation, Macrophages, Microglia, N-Formylmethionine Leucyl-Phenylalanine, Nerve Tissue Proteins, Neuraminidase, Neutrophil Activation, Neutrophils, Peroxisomes, Phylogeny, Polymorphism, Single Nucleotide, Protein Interaction Domains and Motifs, Protein Isoforms, Protein Sorting Signals, Protein Transport, Sialic Acid Binding Ig-like Lectin 3, Alzheimer disease, CD33, Siglec-3, alternative splicing, intracellular trafficking, peroxisome, sialic acid, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

The immunomodulatory receptor Siglec-3/CD33 influences risk for late-onset Alzheimer's disease (LOAD), an apparently human-specific post-reproductive disease. CD33 generates two splice variants: a full-length CD33M transcript produced primarily by the "LOAD-risk" allele and a shorter CD33m isoform lacking the sialic acid-binding domain produced primarily from the "LOAD-protective" allele. An SNP that modulates CD33 splicing to favor CD33m is associated with enhanced microglial activity. Individuals expressing more protective isoform accumulate less brain β-amyloid and have a lower LOAD risk. How the CD33m isoform increases β-amyloid clearance remains unknown. We report that the protection by the CD33m isoform may not be conferred by what it does but, rather, from what it cannot do. Analysis of blood neutrophils and monocytes and a microglial cell line revealed that unlike CD33M, the CD33m isoform does not localize to cell surfaces; instead, it accumulates in peroxisomes. Cell stimulation and activation did not mobilize CD33m to the surface. Thus, the CD33m isoform may neither interact directly with amyloid plaques nor engage in cell-surface signaling. Rather, production and localization of CD33m in peroxisomes is a way of diminishing the amount of CD33M and enhancing β-amyloid clearance. We confirmed intracellular localization by generating a CD33m-specific monoclonal antibody. Of note, CD33 is the only Siglec with a peroxisome-targeting sequence, and this motif emerged by convergent evolution in toothed whales, the only other mammals with a prolonged post-reproductive lifespan. The CD33 allele that protects post-reproductive individuals from LOAD may have evolved by adaptive loss-of-function, an example of the less-is-more hypothesis.

Published
2017

12. Human‐specific polymorphic pseudogenization of SIGLEC12 protects against advanced cancer progression

Author

Shoib S Siddiqui, Michael Vaill, Raymond Do, Naazneen Khan, Andrea L Verhagen, Wu Zhang, Heinz‐Josef Lenz, Teresa L Johnson‐Pais, Robin J Leach, Gary Fraser, Charles Wang, Gen‐Sheng Feng, Nissi Varki, and Ajit Varki

Subjects
advanced carcinoma, dot blot, immunohistochemistry, pseudogenization, SIGLEC12, Biology (General), QH301-705.5
Abstract

Abstract Compared with our closest living evolutionary cousins, humans appear unusually prone to develop carcinomas (cancers arising from epithelia). The SIGLEC12 gene, which encodes the Siglec‐XII protein expressed on epithelial cells, has several uniquely human features: a fixed homozygous missense mutation inactivating its natural ligand recognition property; a polymorphic frameshift mutation eliminating full‐length protein expression in ~60%–70% of worldwide human populations; and, genomic features suggesting a negative selective sweep favoring the pseudogene state. Despite the loss of canonical sialic acid binding, Siglec‐XII still recruits Shp2 and accelerates tumor growth in a mouse model. We hypothesized that dysfunctional Siglec‐XII facilitates human carcinoma progression, correlating with known tumorigenic signatures of Shp2‐dependent cancers. Immunohistochemistry was used to detect Siglec‐XII expression on tissue microarrays. PC‐3 prostate cancer cells were transfected with Siglec‐XII and transcription of genes enriched with Siglec‐XII was determined. Genomic SIGLEC12 status was determined for four different cancer cohorts. Finally, a dot blot analysis of human urinary epithelial cells was established to determine the Siglec‐XII expressors versus non‐expressors. Forced expression in a SIGLEC12 null carcinoma cell line enriched transcription of genes associated with cancer progression. While Siglec‐XII was detected as expected in ~30%–40% of normal epithelia, ~80% of advanced carcinomas showed strong expression. Notably, >80% of late‐stage colorectal cancers had a functional SIGLEC12 allele, correlating with overall increased mortality. Thus, advanced carcinomas are much more likely to occur in individuals whose genomes have an intact SIGLEC12 gene, likely because the encoded Siglec‐XII protein recruits Shp2‐related oncogenic pathways. The finding has prognostic, diagnostic, and therapeutic implications.

Published
2021
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13. Innate extracellular Hsp70 inflammatory properties are mediated by the interaction of Siglec-E and LOX-1 receptors

Author

Borges, Thiago J., primary, Lima, Karina, additional, Murshid, Ayesha, additional, Lape, Isadora T., additional, Zhao, Yunlong, additional, Rigo, Maurício M., additional, Lang, Benjamin J., additional, Siddiqui, Shoib S., additional, Hui, Enfu, additional, Riella, Leonardo V., additional, Bonorino, Cristina, additional, and Calderwood, Stuart K, additional

Published
2023
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16. Syrians' awareness of cardiovascular disease risk factors and warning indicators : a descriptive cross-sectional study

Author

Swed, S., Alibrahim, H., Bohsas, H., Hafez, W., Rais, M. A., Shoib, S., Albazee, E., Elsayed, M. E. G., Sawaf, B., Farwati, A., Seijari, M. N., Battikh, N., Shaheen, N., Ibrahem, N., Alsaleh, A., Lee, Ka Yiu, Rakab, A., Swed, S., Alibrahim, H., Bohsas, H., Hafez, W., Rais, M. A., Shoib, S., Albazee, E., Elsayed, M. E. G., Sawaf, B., Farwati, A., Seijari, M. N., Battikh, N., Shaheen, N., Ibrahem, N., Alsaleh, A., Lee, Ka Yiu, and Rakab, A.

Abstract

The awareness of cardiovascular diseases (CVDs) contributes to the complications and fatality rates from these diseases among individuals; however, no previous study in Syria was conducted on this topic; thus, this study aims to assess Syrians' awareness of CVDs warning symptoms and risk factors. This online cross-sectional study was performed in Syria between the 1st and 25th of August 2022. The inclusion criteria for the sample were citizens of Syria over 18 who currently reside in Syria. The questionnaire included open- and closed-ended questions to assess the awareness of CVDs. A total of 1201 participants enrolled in the study with a response rate of 97.2%; more than half of the participants (61.4%) were aged 18–24. The most recognizable risk factors and warning signs when asking close-ended and open-ended questions were smoking (95.2%, 37.1%) and chest pain (87.8%, 24.8%), respectively. Overall knowledge scores for risk factors and warning signs were (61.5%). Regarding knowledge score of CVDs risk factors and warning signs, participants aged 45–54 scored higher than other age groups, and respondents with a university education level had a higher score than other educational levels (15.7 ± 0.3), (14.5 ± 0.1), respectively. Participants aged 45–54 have a higher probability of good knowledge of CVDs risk factors and warning signs than participants aged 18–24 (OR = 4.8, P value < 0.001), while participants living in the countryside were less likely to have good knowledge of CVDs risk factors and warning signs than city residents (OR = 0.6, P value < 0.05). According to our results, there is inadequate knowledge of the risk factors and warning signs of CVDs. Consequently, there is a greater need to raise CVD awareness and learning initiatives on the disease's risk factors and symptoms., Correction to: Scientific Reports 10.1038/s41598-023-35321-2

Published
2023
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17. Monkeypox in Syria : Highlighting an awareness issue

Author

Swed, S., Alibrahim, H., Bohsas, H., Aljabali, A., Almoshantaf, M. B., Sawaf, B., Shoib, S., Patwary, M. M., Albazee, E., Lee, Ka Yiu, Farwati, A., Seijari, M. N., Hafez, W., Rakab, A., Swed, S., Alibrahim, H., Bohsas, H., Aljabali, A., Almoshantaf, M. B., Sawaf, B., Shoib, S., Patwary, M. M., Albazee, E., Lee, Ka Yiu, Farwati, A., Seijari, M. N., Hafez, W., and Rakab, A.

Abstract

Background: The World Health Organization (WHO) verified 780 cases of monkeypox across 27 countries between 13 May 2022 and 2 June 2022. The aim of our study was to assess the level of awareness of human monkeypox virus among Syrian medical students, general practitioners, medical residents, and specialists. Methods: A cross-sectional online survey was performed in Syria between May 2 and September 8, 2022. The survey consisted of 53 questions within the following three categories: demographic information, work-related details, and monkeypox knowledge. Results: In total, 1257 Syrian healthcare workers and medical students were enrolled in our study. The animal host and incubation time for monkeypox were correctly identified by just 2.7% and 33.3% of responders, respectively. Sixty percent of the study sample thought that the symptoms of monkeypox and smallpox are identical. No statistically significant associations were found between predictor variables and knowledge regarding monkeypox (p-value > 0.05). Conclusion: Education and awareness regarding monkeypox vaccinations are of paramount importance. It is essential that clinical doctors are adequately aware of this disease, in order to avoid an uncontrolled situation, as experienced with COVID-19.

Published
2023
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22. Human‐specific polymorphic pseudogenization of SIGLEC12 protects against advanced cancer progression

Author

Raymond Do, Charles Wang, Ajit Varki, Nissi Varki, Robin J. Leach, Michael Vaill, Naazneen Khan, Wu Zhang, Gen-Sheng Feng, Andrea Verhagen, Gary E. Fraser, Heinz-Josef Lenz, Shoib S. Siddiqui, and Teresa L. Johnson-Pais

Subjects
Cancer Research, Tissue microarray, Physiology, Pseudogene, Cancer, Sialic acid binding, respiratory system, Biology, medicine.disease, Biochemistry, Genetics and Molecular Biology (miscellaneous), Frameshift mutation, advanced carcinoma, dot blot, SIGLEC12, lcsh:Biology (General), immunohistochemistry, Cancer research, medicine, Molecular Medicine, Missense mutation, pseudogenization, Allele, lcsh:QH301-705.5, Gene
Abstract

Compared with our closest living evolutionary cousins, humans appear unusually prone to develop carcinomas (cancers arising from epithelia). The SIGLEC12 gene, which encodes the Siglec‐XII protein expressed on epithelial cells, has several uniquely human features: a fixed homozygous missense mutation inactivating its natural ligand recognition property; a polymorphic frameshift mutation eliminating full‐length protein expression in ~60%–70% of worldwide human populations; and, genomic features suggesting a negative selective sweep favoring the pseudogene state. Despite the loss of canonical sialic acid binding, Siglec‐XII still recruits Shp2 and accelerates tumor growth in a mouse model. We hypothesized that dysfunctional Siglec‐XII facilitates human carcinoma progression, correlating with known tumorigenic signatures of Shp2‐dependent cancers. Immunohistochemistry was used to detect Siglec‐XII expression on tissue microarrays. PC‐3 prostate cancer cells were transfected with Siglec‐XII and transcription of genes enriched with Siglec‐XII was determined. Genomic SIGLEC12 status was determined for four different cancer cohorts. Finally, a dot blot analysis of human urinary epithelial cells was established to determine the Siglec‐XII expressors versus non‐expressors. Forced expression in a SIGLEC12 null carcinoma cell line enriched transcription of genes associated with cancer progression. While Siglec‐XII was detected as expected in ~30%–40% of normal epithelia, ~80% of advanced carcinomas showed strong expression. Notably, >80% of late‐stage colorectal cancers had a functional SIGLEC12 allele, correlating with overall increased mortality. Thus, advanced carcinomas are much more likely to occur in individuals whose genomes have an intact SIGLEC12 gene, likely because the encoded Siglec‐XII protein recruits Shp2‐related oncogenic pathways. The finding has prognostic, diagnostic, and therapeutic implications.

Published
2020

23. Natural compound catechol induces <scp>DNA</scp> damage, apoptosis, and <scp>G1</scp> cell cycle arrest in breast cancer cells

Author

John Marton, Varsha Menon, Raafat El-Awady, Rachel Matar, Shoib S. Siddiqui, Rajan Radhakrishnan, Cijo George Vazhappilly, Amina Jamal Laham, Rawad Hodeify, Hussain Al Zouabi, and Maxime Merheb

Subjects
Programmed cell death, Cyclin E, DNA damage, Catechols, Apoptosis, Breast Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Humans, skin and connective tissue diseases, Cytotoxicity, Pharmacology, 0303 health sciences, Chemistry, 030302 biochemistry & molecular biology, Cell cycle, G1 Phase Cell Cycle Checkpoints, 030220 oncology & carcinogenesis, Cancer research, Female, Signal transduction, G1 phase, DNA Damage, Signal Transduction
Abstract

Targeting cell cycle and inducing DNA damage by activating cell death pathways are considered as effective therapeutic strategy for combating breast cancer progression. Many of the naturally known small molecules target these signaling pathways and are effective against resistant and/or aggressive types of breast cancers. Here, we investigated the effect of catechol, a naturally occurring plant compound, for its specificity and chemotherapeutic efficacies in breast cancer (MCF-7 and MDA-MB-231) cells. Catechol treatment showed concentration-dependent cytotoxicity and antiproliferative growth in both MCF-7 and MDA-MB-231 cells while sparing minimal effects on noncancerous (F-180 and HK2) cells. Catechol modulated differential DNA damage effects by activating ATM/ATR pathways and showed enhanced γ-H2AX expression, as an indicator for DNA double-stranded breaks. MCF-7 cells showed G1 cell cycle arrest by regulating p21-mediated cyclin E/Cdk2 inhibition. Furthermore, activation of p53 triggered a caspase-mediated cell death mechanism by inhibiting regulatory proteins such as DNMT1, p-BRCA1, MCL-1, and PDCD6 with an increased Bax/Bcl-2 ratio. Overall, our results showed that catechol possesses favorable safety profile for noncancerous cells while specifically targeting multiple signaling cascades to inhibit proliferation in breast cancer cells.

Published
2020

24. A multinational Delphi consensus to end the COVID-19 public health threat

Author

Lazarus, J. V., Romero, D., Kopka, C. J., Karim, S. A., Abu-Raddad, L. J., Almeida, G., Baptista-Leite, R., Barocas, J. A., Barreto, M. L., Bar-Yam, Y., Bassat, Q., Batista, C., Bazilian, M., Chiou, S. -T., del Rio, C., Dore, G. J., Gao, G. F., Gostin, L. O., Hellard, M., Jimenez, J. L., Kang, G., Lee, N., Maticic, M., Mckee, M., Nsanzimana, S., Oliu-Barton, M., Pradelski, B., Pyzik, O., Rabin, K., Raina, S., Rashid, S. F., Rathe, M., Saenz, R., Singh, S., Trock-Hempler, M., Villapol, S., Yap, P., Binagwaho, A., Kamarulzaman, A., El-Mohandes, A., Barreto, M., Abdulla, S., Addleman, S., Aghayeva, G., Agius, R., Ahmed, M., Ramy, M. A., Aide, P., Aleman, S., Alfred, J. -P., Ali, S., Aliaga, J., Aloudat, T., Alqahtani, S. A., Al-Salman, J., Amuasi, J. H., Agrawal, A., Anwar, W., Araujo-Jorge, T., Artaza, O., Asadi, L., Awuku, Y., Baker, M., Barberia, L., Bascolo, E., Belcher, P., Bell, L., Benzaken, A., Bergholtz, E., Bhadelia, N., Bhan, A., Bilodeau, S., Bitran, R., Bluyssen, P., Bosman, A., Bozza, F. A., Brinkmann, M. M., Brown, A., Mellado, B., Bukusi, E., Bullen, C., Buonanno, G., Burgess, R., Butler, M., Byakika-Kibwika, P., Cabieses, B., Carlsson, G., Cascini, Fidelia, Chabala, C., Chakroun, M., Cheng, K. K., Chetty, A., Chumachenko, D., Consalves, G., Conway Morris, A., Cordie, A., Corrah, T., Crabtree-Ramirez, B., Dashdorj, N., Davidovitch, N., de Souza, L. E., Dhariwal, A. C., Druica, E., Ergonul, O., Erondu, N. A., Essar, M. Y., Ewing, A., Fanjul, G., Feierstein, D., Feigl-Ding, E., Figueroa, R., Figueroa, J. P., Fisher, D., Flores, W., Forero-Pena, D. A., Frumkin, H., Gamkrelidze, A., Gandhi, M., Garcia, P., Garcia-Basteiro, A. L., Garcia-Sastre, A., Garg, S., Gbeasor-Komlanvi, F. A., Gershenson, C., Gilada, I., Giovanella, L., Gonzalez, M., Green, M. S., Greenhalgh, T., Griffin, P., Griffin, S., Grinsztejn, B., Anand, T., Guerra, G., Guinto, R., Gujski, M., Guner, R., Hamdy, A., Hancean, M. -G., Haniffa, A., Hartigan-Go, K. Y., Hassan, H. K., Hay, S. I., Heino, M. T. J., Hel, Z., Hotez, P., Hu, J., Hukic, M., Ijsselmuiden, C., Iroko, D., Iskarous, M., Izugbara, C., Jacobs, C., Jadad, A. R., Jehan, F., Jordan, A., Jroundi, I., Kain, K., Kamberi, F., Karamov, E., Karan, A., Katz, R., Katzourakis, A., Kazembe, A., Khamis, F., Khamzayev, K., Khanyola, J., Khunti, K., Kiguli-Malwadde, E., Kim, W. J., Kirenga, B. J., Klimovsky, D., Kmush, B. L., Knaul, F., Kogevinas, M., Kristensen, F., Kumar, D., Kumar, R., Kvalsvig, A., Lacerda, M. V., Lal, A., Lawton, T., Lemery, J., Leonardi, A. J., Li, Y., Lottvall, J., Lounis, M., Maceira, D., Macintyre, C. R., Madani, A., Magiorkinis, G., Malekzadeh, R., Choisy, M., Marcelin, J. R., Marks, G. B., Marr, L., Marrazzo, J., Martina, A., Martin-Moreno, J. M., Mateos, C., Mayxay, M., Mazarati, J. B., Mboup, S., Mcdonald, J., Mcmillan, F., Mechili, E., Medici, A., Davis, S. L. M., Meier, P., Memish, Z. A., Menon, J., Menon, P., Mesiano-Crookston, J., Michie, S., Mikolasevic, I., Milicevic, O., Mishra, A. K., Mohamed, R., Mokdad, A. H., Monroy-Valle, M., Morawska, L., Moschos, S. A., Motawea, K., Mousavi, S. H., Mumtaz, G., Munene, P. K., Munoz Almagro, C., Muriuki, J., Muyingo, S., Naniche, D., Naylor, C. D., Ndembi, N., Nemec, J., Nesteruk, I., Ngaruiya, C., Nguyen, H., Nikolova, D., Nitzan, D., Norheim, O., Noushad, M., Ntoumi, F., Nyborg, G. A., Ochodo, E., Odabasi, Z., Okwen, M. P., Olivia, K., Ong, D. S. Y., Opara, I., Orozco, M., Oshitani, H., Pagel, C., Pai, M., Palsdottir, B., Papatheodoridis, G., Paraskevis, D., Leigh, J. P., Pecoul, B., Peichl, A., Perez-Then, E., Duc, P. P., Philippe, C., Pineda Rojas, A., Pladsen, C., Pozniak, A., Quiroga, R., Qureshi, H., Rampal, S., Ranney, M., Rathe, L., Ratzan, S., Raventos, H., Rees, H., Reis, R., Ricciardi, Walter, Rizk, N., Robalo, M., Robertson, E., Robinson, L., Rokx, C., Ros, T., Rottingen, J. -A., Rubin, M., Ruxrungtam, K., Sadirova, S., Saha, S., Salgado, N., Sanchez, L., Sangaramoorthy, T., Santamaria-Ulloa, C., Santos, R., Sawaf, B., Schneider, M. F., Schooley, R. T., Sener, A., Sepulveda, J., Shah, J., Shibani, M., Shoib, S., Sikazwe, I., Simaitis, A., Gill, A. S., Skhvitaridze, N., Sokolovic, M., Solomon, R., Solorzano, X., Springer, S. A., Srol, J., Staines, A., Stelfox, H. T., Strathdee, S., Sulaiman, L. H., Sutton, B., Svanaes, D., Swed, S., Sypsa, V., Sorensen, K., Tajudeen, R., Tan, A., Tang, J., Tanner, M., Sethi, T., Temmerman, M., Than, K. K., Tinto, H., Tometissi, S. P., Torres, I., Tshering, K. P., Tsiodras, S., Tsofa, B., Vahlne, A., Vargas, J. R., Bernal, I. D. V., Ventura, D., Vilasanjuan, R., Vipond, J., Wamala-Andersson, S., Wargocki, P., West, R., Weyand, A., White, T. M., Wolff, G., Yao, M., Yates, C. A., Yeboah, G., Yee-Sin, L., Yi, S., Teo, Y. -Y., Yong, P., Zamora-Mesia, V., Ovrehus, A., Cascini F. (ORCID:0000-0001-6499-0734), Ricciardi W. (ORCID:0000-0002-5655-688X), Lazarus, J. V., Romero, D., Kopka, C. J., Karim, S. A., Abu-Raddad, L. J., Almeida, G., Baptista-Leite, R., Barocas, J. A., Barreto, M. L., Bar-Yam, Y., Bassat, Q., Batista, C., Bazilian, M., Chiou, S. -T., del Rio, C., Dore, G. J., Gao, G. F., Gostin, L. O., Hellard, M., Jimenez, J. L., Kang, G., Lee, N., Maticic, M., Mckee, M., Nsanzimana, S., Oliu-Barton, M., Pradelski, B., Pyzik, O., Rabin, K., Raina, S., Rashid, S. F., Rathe, M., Saenz, R., Singh, S., Trock-Hempler, M., Villapol, S., Yap, P., Binagwaho, A., Kamarulzaman, A., El-Mohandes, A., Barreto, M., Abdulla, S., Addleman, S., Aghayeva, G., Agius, R., Ahmed, M., Ramy, M. A., Aide, P., Aleman, S., Alfred, J. -P., Ali, S., Aliaga, J., Aloudat, T., Alqahtani, S. A., Al-Salman, J., Amuasi, J. H., Agrawal, A., Anwar, W., Araujo-Jorge, T., Artaza, O., Asadi, L., Awuku, Y., Baker, M., Barberia, L., Bascolo, E., Belcher, P., Bell, L., Benzaken, A., Bergholtz, E., Bhadelia, N., Bhan, A., Bilodeau, S., Bitran, R., Bluyssen, P., Bosman, A., Bozza, F. A., Brinkmann, M. M., Brown, A., Mellado, B., Bukusi, E., Bullen, C., Buonanno, G., Burgess, R., Butler, M., Byakika-Kibwika, P., Cabieses, B., Carlsson, G., Cascini, Fidelia, Chabala, C., Chakroun, M., Cheng, K. K., Chetty, A., Chumachenko, D., Consalves, G., Conway Morris, A., Cordie, A., Corrah, T., Crabtree-Ramirez, B., Dashdorj, N., Davidovitch, N., de Souza, L. E., Dhariwal, A. C., Druica, E., Ergonul, O., Erondu, N. A., Essar, M. Y., Ewing, A., Fanjul, G., Feierstein, D., Feigl-Ding, E., Figueroa, R., Figueroa, J. P., Fisher, D., Flores, W., Forero-Pena, D. A., Frumkin, H., Gamkrelidze, A., Gandhi, M., Garcia, P., Garcia-Basteiro, A. L., Garcia-Sastre, A., Garg, S., Gbeasor-Komlanvi, F. A., Gershenson, C., Gilada, I., Giovanella, L., Gonzalez, M., Green, M. S., Greenhalgh, T., Griffin, P., Griffin, S., Grinsztejn, B., Anand, T., Guerra, G., Guinto, R., Gujski, M., Guner, R., Hamdy, A., Hancean, M. -G., Haniffa, A., Hartigan-Go, K. Y., Hassan, H. K., Hay, S. I., Heino, M. T. J., Hel, Z., Hotez, P., Hu, J., Hukic, M., Ijsselmuiden, C., Iroko, D., Iskarous, M., Izugbara, C., Jacobs, C., Jadad, A. R., Jehan, F., Jordan, A., Jroundi, I., Kain, K., Kamberi, F., Karamov, E., Karan, A., Katz, R., Katzourakis, A., Kazembe, A., Khamis, F., Khamzayev, K., Khanyola, J., Khunti, K., Kiguli-Malwadde, E., Kim, W. J., Kirenga, B. J., Klimovsky, D., Kmush, B. L., Knaul, F., Kogevinas, M., Kristensen, F., Kumar, D., Kumar, R., Kvalsvig, A., Lacerda, M. V., Lal, A., Lawton, T., Lemery, J., Leonardi, A. J., Li, Y., Lottvall, J., Lounis, M., Maceira, D., Macintyre, C. R., Madani, A., Magiorkinis, G., Malekzadeh, R., Choisy, M., Marcelin, J. R., Marks, G. B., Marr, L., Marrazzo, J., Martina, A., Martin-Moreno, J. M., Mateos, C., Mayxay, M., Mazarati, J. B., Mboup, S., Mcdonald, J., Mcmillan, F., Mechili, E., Medici, A., Davis, S. L. M., Meier, P., Memish, Z. A., Menon, J., Menon, P., Mesiano-Crookston, J., Michie, S., Mikolasevic, I., Milicevic, O., Mishra, A. K., Mohamed, R., Mokdad, A. H., Monroy-Valle, M., Morawska, L., Moschos, S. A., Motawea, K., Mousavi, S. H., Mumtaz, G., Munene, P. K., Munoz Almagro, C., Muriuki, J., Muyingo, S., Naniche, D., Naylor, C. D., Ndembi, N., Nemec, J., Nesteruk, I., Ngaruiya, C., Nguyen, H., Nikolova, D., Nitzan, D., Norheim, O., Noushad, M., Ntoumi, F., Nyborg, G. A., Ochodo, E., Odabasi, Z., Okwen, M. P., Olivia, K., Ong, D. S. Y., Opara, I., Orozco, M., Oshitani, H., Pagel, C., Pai, M., Palsdottir, B., Papatheodoridis, G., Paraskevis, D., Leigh, J. P., Pecoul, B., Peichl, A., Perez-Then, E., Duc, P. P., Philippe, C., Pineda Rojas, A., Pladsen, C., Pozniak, A., Quiroga, R., Qureshi, H., Rampal, S., Ranney, M., Rathe, L., Ratzan, S., Raventos, H., Rees, H., Reis, R., Ricciardi, Walter, Rizk, N., Robalo, M., Robertson, E., Robinson, L., Rokx, C., Ros, T., Rottingen, J. -A., Rubin, M., Ruxrungtam, K., Sadirova, S., Saha, S., Salgado, N., Sanchez, L., Sangaramoorthy, T., Santamaria-Ulloa, C., Santos, R., Sawaf, B., Schneider, M. F., Schooley, R. T., Sener, A., Sepulveda, J., Shah, J., Shibani, M., Shoib, S., Sikazwe, I., Simaitis, A., Gill, A. S., Skhvitaridze, N., Sokolovic, M., Solomon, R., Solorzano, X., Springer, S. A., Srol, J., Staines, A., Stelfox, H. T., Strathdee, S., Sulaiman, L. H., Sutton, B., Svanaes, D., Swed, S., Sypsa, V., Sorensen, K., Tajudeen, R., Tan, A., Tang, J., Tanner, M., Sethi, T., Temmerman, M., Than, K. K., Tinto, H., Tometissi, S. P., Torres, I., Tshering, K. P., Tsiodras, S., Tsofa, B., Vahlne, A., Vargas, J. R., Bernal, I. D. V., Ventura, D., Vilasanjuan, R., Vipond, J., Wamala-Andersson, S., Wargocki, P., West, R., Weyand, A., White, T. M., Wolff, G., Yao, M., Yates, C. A., Yeboah, G., Yee-Sin, L., Yi, S., Teo, Y. -Y., Yong, P., Zamora-Mesia, V., Ovrehus, A., Cascini F. (ORCID:0000-0001-6499-0734), and Ricciardi W. (ORCID:0000-0002-5655-688X)

Abstract

Despite notable scientific and medical advances, broader political, socioeconomic and behavioural factors continue to undercut the response to the COVID-19 pandemic1,2. Here we convened, as part of this Delphi study, a diverse, multidisciplinary panel of 386 academic, health, non-governmental organization, government and other experts in COVID-19 response from 112 countries and territories to recommend specific actions to end this persistent global threat to public health. The panel developed a set of 41 consensus statements and 57 recommendations to governments, health systems, industry and other key stakeholders across six domains: communication; health systems; vaccination; prevention; treatment and care; and inequities. In the wake of nearly three years of fragmented global and national responses, it is instructive to note that three of the highest-ranked recommendations call for the adoption of whole-of-society and whole-of-government approaches1, while maintaining proven prevention measures using a vaccines-plus approach2 that employs a range of public health and financial support measures to complement vaccination. Other recommendations with at least 99% combined agreement advise governments and other stakeholders to improve communication, rebuild public trust and engage communities3 in the management of pandemic responses. The findings of the study, which have been further endorsed by 184 organizations globally, include points of unanimous agreement, as well as six recommendations with >5% disagreement, that provide health and social policy actions to address inadequacies in the pandemic response and help to bring this public health threat to an end.

Published
2022

25. Armed assault of Russia on Ukraine and looming danger on regional mental health: a call for action by psychiatrists in conflict settings

Author

Shoib, S., Armiya'u, A., Chandradasa, M., Жаркова, Альбiна Володимирiвна, Zharkova, Albina Volodymyrivna, Kolesnyk, P., Swed, S., and Lucero-Prisno, D.

Subjects
ongoing armed conflict, Russian-Ukrainian socio-political relationship, social wellbeing, annexation of Crimea, mental health
Abstract

The Russian-Ukrainian socio-political relationship is embroiled in centuries of conflicts, bloodshed and brutal invasions. The modern dissension dates back to the 2014 annexation of Crimea by Russia in the aftermath of the Ukrainian Revolution of Dignity and has been escalating rapidly during the recent months. The tensions between the two nations have boiled over to the Russian forces entering Ukrainian soil from the North, South, and East on 24 February 2022. This puts the lives of millions of people at risk, particularly those residing in Eastern Ukraine who are estimated to be around 14 million people and also residents of major cities in other parts of the country (Ukraine, 2022). The ongoing armed conflict will have a deleterious impact on their mental health and social wellbeing. The fear of further armed aggression will force people to leave their homes and will lead to dire mental health consequences (Jazeera, Reference Jazeera2022).

Published
2022

26. Current state of cannabis use, policies, and research across sixteen countries: cross-country comparisons and international perspectives

Author

Ransing, R. (Ramdas), Rosa-Fernández-Pacheco, F.J. (Francisco Javier) de la, Pereira-Sánchez, V. (Víctor), Handuleh, J.I.M. (Jibril I. M.), Jerotic, S. (Stefan), Gupta, A.K. (Anoop Krishna), Karaliuniene, R. (Ruta), Filippis, R. (Renato) de, Peyron, E. (Eric), Sonmez-Gungor, E. (Ekin), Boujraf, S. (Said), Yee, A. (Ane), Vahdani, B. (Bita), Shoib, S. (Sheikh), Stowe, M.J. (M.J.), Jaguga, F. (Florence), Dannatt, L. (Lisa), da-Silva, A.K. (Alexandre Kieslich), Grandinetti, P. (Paolo), and Jatchavala, C. (Chonnakarn)

Subjects
Research, Global health, Legalization, Área Psicología, Policies, Cannabis
Abstract

Introduction: Varying public views on cannabis use across countries may explain the variation in the prevalence of use, policies, and research in individual countries, and global regulation of cannabis. This paper aims to describe the current state of cannabis use, policies, and research across sixteen countries.Methods: PubMed and Google Scholar were searched for studies published from 2010 to 2020. Searches were conducted using the relevant country of interest as a search term (e.g., "Iran"), as well as relevant predefined keywords such as "cannabis," "marijuana," "hashish," "bhang "dual diagnosis," "use," "addiction," "prevalence," "co-morbidity," "substance use disorder," "legalization" or "policy" (in English and non-English languages). These keywords were used in multiple combinations to create the search string for studies' titles and abstracts. Official websites of respective governments and international organizations were also searched in English and non-English languages (using countries national languages) to identify the current state of cannabis use, policies, and research in each of those countries.Results: The main findings were inconsistent and heterogeneous reporting of cannabis use, variation in policies (e.g., legalization), and variation in intervention strategies across the countries reviewed. European countries dominate the cannabis research output indexed on PubMed, in contrast to Asian countries (Thailand, Malaysia, India, Iran, and Nepal).Conclusions: Although global cannabis regulation is ongoing, the existing heterogeneities across countries in terms of policies and epidemiology can increase the burden of cannabis use disorders disproportionately and unpredictably. There is an urgent need to develop global strategies to address these cross-country barriers to improve early detection, prevention, and interventions for cannabis use and related disorders.

Published
2022

31. Dual actions of group B Streptococcus capsular sialic acid provide resistance to platelet-mediated antimicrobial killing

Author

Shoib S. Siddiqui, Jamey D. Marth, Kyoko Fukahori, Ajit Varki, Josh Sun, Nao Ando, Satoshi Uchiyama, Flavio Schwarz, Mengyou Wu, and Victor Nizet

Subjects
0301 basic medicine, Multidisciplinary, Innate immune system, Antimicrobial peptides, SIGLEC, Microbiology, Sialic acid, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Immune system, chemistry, Immunity, 030220 oncology & carcinogenesis, bacteria, Platelet, Platelet activation
Abstract

Circulating platelets have important functions in thrombosis and in modulating immune and inflammatory responses. However, the role of platelets in innate immunity to bacterial infection is largely unexplored. While human platelets rapidly kill Staphylococcus aureus, we found the neonatal pathogen group B Streptococcus (GBS) to be remarkably resistant to platelet killing. GBS possesses a capsule polysaccharide (CPS) with terminal α2,3-linked sialic acid (Sia) residues that mimic a common epitope present on the human cell surface glycocalyx. A GBS mutant deficient in CPS Sia was more efficiently killed by human platelets, thrombin-activated platelet releasate, and synthetic platelet-associated antimicrobial peptides. GBS Sia is known to bind inhibitory Sia-recognizing Ig superfamily lectins (Siglecs) to block neutrophil and macrophage activation. We show that human platelets also express high levels of inhibitory Siglec-9 on their surface, and that GBS can engage this receptor in a Sia-dependent manner to suppress platelet activation. In a mouse i.v. infection model, antibody-mediated platelet depletion increased susceptibility to platelet-sensitive S. aureus but did not alter susceptibility to platelet-resistant GBS. Elimination of murine inhibitory Siglec-E partially reversed platelet suppression in response to GBS infection. We conclude that GBS Sia has dual roles in counteracting platelet antimicrobial immunity: conferring intrinsic resistance to platelet-derived antimicrobial components and inhibiting platelet activation through engagement of inhibitory Siglecs. We report a bacterial virulence factor for evasion of platelet-mediated innate immunity.

Published
2019

32. Evolutionary conservation of human ketodeoxynonulosonic acid production is independent of sialoglycan biosynthesis

Author

Kunio Kawanishi, Shoib S. Siddiqui, Sudeshna Saha, Ken Kitajima, Xi Chen, Kumar Sharma, Ian C. Schoenhofen, Biswa Choudhury, Aniruddha Sasmal, Ajit Varki, Anja K. Münster-Kühnel, Sandra Diaz, Michael Vaill, Chihiro Sato, and Hudson H. Freeze

Subjects
0301 basic medicine, Glycan, Glycosylation, Immunology, Glycobiology, Mannose, Medical and Health Sciences, Kidney Failure, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Biosynthesis, Polysaccharides, Human Umbilical Vein Endothelial Cells, 2.1 Biological and endogenous factors, Humans, Chronic, Aetiology, chemistry.chemical_classification, Methionine, biology, General Medicine, Atherosclerosis, N-Acetylneuraminic Acid, Sialic acid, 030104 developmental biology, Enzyme, Metabolism, HEK293 Cells, chemistry, Biochemistry, Nephrology, 030220 oncology & carcinogenesis, biology.protein, Kidney Failure, Chronic, Research Article
Abstract

Human metabolic incorporation of nonhuman sialic acid (Sia) N-glycolylneuraminic acid into endogenous glycans generates inflammation via preexisting antibodies, which likely contributes to red meat–induced atherosclerosis acceleration. Exploring whether this mechanism affects atherosclerosis in end-stage renal disease (ESRD), we instead found serum accumulation of 2-keto-3-deoxy-d-glycero-d-galacto-2-nonulosonic acid (Kdn), a Sia prominently expressed in cold-blooded vertebrates. In patients with ESRD, levels of the Kdn precursor mannose also increased, but within a normal range. Mannose ingestion by healthy volunteers raised the levels of urinary mannose and Kdn. Kdn production pathways remained conserved in mammals but were diminished by an M42T substitution in a key biosynthetic enzyme, N-acetylneuraminate synthase. Remarkably, reversion to the ancestral methionine then occurred independently in 2 lineages, including humans. However, mammalian glycan databases contain no Kdn-glycans. We hypothesize that the potential toxicity of excess mannose in mammals is partly buffered by conversion to free Kdn. Thus, mammals probably conserve Kdn biosynthesis and modulate it in a lineage-specific manner, not for glycosylation, but to control physiological mannose intermediates and metabolites. However, human cells can be forced to express Kdn-glycans via genetic mutations enhancing Kdn utilization, or by transfection with fish enzymes producing cytidine monophosphate–Kdn (CMP-Kdn). Antibodies against Kdn-glycans occur in pooled human immunoglobulins. Pathological conditions that elevate Kdn levels could therefore result in antibody-mediated inflammatory pathologies.

Published
2021

33. Sialoglycan recognition is a common connection linking acidosis, zinc, and HMGB1 in sepsis

Author

Chirag Dhar, Ajit Varki, Xiaoxiao Zhang, Venkatasubramaniam Sundaramurthy, Shoib S. Siddiqui, Miaomiao Li, Ding Xu, Hai Yu, Aniruddha Sasmal, Xi Chen, Esther Bandala-Sanchez, and Leonard C. Harrison

Subjects
Lipopolysaccharides, Sialoglycoproteins, chemistry.chemical_element, chemical and pharmacologic phenomena, Zinc, HMGB1, Divalent, Sepsis, chemistry.chemical_compound, Immunology and Inflammation, Polysaccharides, medicine, Humans, Innate, HMGB1 Protein, Whole blood, Acidosis, chemistry.chemical_classification, Multidisciplinary, biology, Inflammatory and immune system, Immunity, COVID-19, Hematology, Biological Sciences, Hydrogen-Ion Concentration, medicine.disease, Immunity, Innate, Lactic acid, Sialic acid, Infectious Diseases, chemistry, Biochemistry, Neu5Ac, sialic acid, cytokine storm, biology.protein, Sialic Acids, medicine.symptom, Carrier Proteins
Abstract

Significance Sepsis is a condition wherein a microbial infection leads to life-threatening systemic hyperactivation of innate immunity. Blood pH is normally maintained tightly between 7.35 and 7.45, and lactic acidosis with a pH, Blood pH is tightly maintained between 7.35 and 7.45, and acidosis (pH

Published
2021

34. Modulation of calcium-binding proteins expression and cisplatin chemosensitivity by calcium chelation in human breast cancer MCF-7 cells

Author

Rawad Hodeify, Cijo George Vazhappilly, John Marton, Shoib S. Siddiqui, Rachel Matar, Hussain Al Zouabi, and Maxime Merheb

Subjects
0301 basic medicine, Calcium-binding proteins, Calmodulin, chemistry.chemical_element, Calcium, Calcium in biology, 03 medical and health sciences, 0302 clinical medicine, Calcium-binding protein, medicine, Viability assay, lcsh:Social sciences (General), lcsh:Science (General), Intracellular calcium, Calcium metabolism, Cisplatin, Multidisciplinary, biology, BAPTA-AM, 030104 developmental biology, MCF-7, chemistry, biology.protein, Cancer research, lcsh:H1-99, 030217 neurology & neurosurgery, lcsh:Q1-390, medicine.drug, Research Article
Abstract

Cisplatin (CDDP) is currently one of the most effective FDA-approved treatments for breast cancer. Previous studies have shown that CDDP-induced cell death in human breast cancer (MCF-7) cells is associated with disruption of calcium homeostasis. However, whether the sensitivity of breast cancer cells to cisplatin is associated with dysregulation of the expression of calcium-binding proteins (CaBPs) remains unknown. In this study, we evaluated the effect of the intracellular calcium chelator (BAPTA-AM) on viability of MCF-7 cells in the presence of toxic and sub-toxic doses of cisplatin. Furthermore, this study assessed the expression of CaBPs, calmodulin, S100A8, and S100A14 in MCF-7 cells treated with cisplatin. Cell viability was determined using MTT-based in vitro toxicity assay. Intracellular calcium imaging was done using Fluo-4 AM, a cell-permeant fluorescent calcium indicator. Expression of CaBPs was tested using real-time quantitative PCR. Exposure of cells to increasing amounts of CDDP correlated with increasing fluorescence of the intracellular calcium indicator, Fluo-4 AM. Conversely, treating cells with cisplatin significantly decreased mRNA levels of calmodulin, S100A8, and S100A14. Treatment of the cells with calcium chelator, BAPTA-AM, significantly enhanced the cytotoxic effects of sub-toxic dose of cisplatin. Our results indicated a statistically significant negative correlation between calmodulin, S100A8, and S100A14 expression and sensitivity of breast cancer cells to a sub-toxic dose of cisplatin. We propose that modulating the activity of calcium-binding proteins, calmodulin, S100A8, and S100A14, could be used to increase cisplatin efficacy, lowering its treatment dosage while maintaining its chemotherapeutic value., Cisplatin; Calcium-binding proteins; BAPTA-AM; Intracellular calcium.

Published
2021

36. Cross-cultural prevalence of sleep quality and psychological distress in healthcare workers during COVID-19 pandemic

Author

Khan, H. R., Ashraf, F., Ullah, I., Tahir, M. J., Dominari, A., Shoib, S., Naeem, H., Reddy, G., Mukherjee, P., Akram, I., Kamada, S., Memon, R. R., Khan, M. M. Y., Raut, S., Shalaby, M. M. M., Anwar, R. U., Farooq, M., Soparia, K. K., Ramalho, R., Lin, C. -Y, Pakpour, Amir H., Khan, H. R., Ashraf, F., Ullah, I., Tahir, M. J., Dominari, A., Shoib, S., Naeem, H., Reddy, G., Mukherjee, P., Akram, I., Kamada, S., Memon, R. R., Khan, M. M. Y., Raut, S., Shalaby, M. M. M., Anwar, R. U., Farooq, M., Soparia, K. K., Ramalho, R., Lin, C. -Y, and Pakpour, Amir H.

Abstract

Background: Poor quality sleep and emotional disturbances are expected in times of crisis. COVID-19 has severely impacted healthcare worldwide and with that comes the concern about its effects on healthcare workers. The purpose of the present study was to assess sleep quality and psychological distress in healthcare workers during the COVID-19 pandemic. Methods: The present work is a multi-centric cross-sectional study targeting healthcare workers from India, Pakistan, and Nepal. It used an online version of the Pittsburg Sleep Quality Index and the General Health Questionnaire, and data were analyzed using SPSS V.24. Results: A total of 1790 participants completed the questionnaire. Of the 1790 participants, 57% reported poor sleep quality, and 10% reported a high level of psychological distress. A cross-cultural comparison found some differences between the different groups of participants. The details of the differences were further explored in the article. Conclusion: The present study highlights that a significant proportion of healthcare workers are affected by poor sleep quality and psychological distress during the COVID-19 pandemic. It also emphasizes the imperative to provide them with psychosocial support to avoid potential short- and long-term psychological consequences of these troubling times.

Published
2021
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37. Internet addiction and sleep quality among medical students during the COVID-19 pandemic : A multinational cross-sectional survey

Author

Tahir, M. J., Malik, N. I., Ullah, I., Khan, H. R., Perveen, S., Ramalho, R., Siddiqi, A. R., Waheed, S., Mohamed Shalaby, M. M., de Berardis, D., Jain, S., Vetrivendan, G. L., Chatterjee, H., Gopar Franco, W. X., Shafiq, M. A., Fatima, N. T., Abeysekera, M., Sayyeda, Q., Shamat, S. F., Aiman, W., Akhtar, Q., Devi, A., Aftab, A., Shoib, S., Lin, C. -Y, Pakpour, Amir H., Tahir, M. J., Malik, N. I., Ullah, I., Khan, H. R., Perveen, S., Ramalho, R., Siddiqi, A. R., Waheed, S., Mohamed Shalaby, M. M., de Berardis, D., Jain, S., Vetrivendan, G. L., Chatterjee, H., Gopar Franco, W. X., Shafiq, M. A., Fatima, N. T., Abeysekera, M., Sayyeda, Q., Shamat, S. F., Aiman, W., Akhtar, Q., Devi, A., Aftab, A., Shoib, S., Lin, C. -Y, and Pakpour, Amir H.

Abstract

Background The emergence of the COVID-19 pandemic has affected the lives of many people, including medical students. The present study explored internet addiction and changes in sleep patterns among medical students during the pandemic and assessed the relationship between them. Methods A cross-sectional study was carried out in seven countries, the Dominican Republic, Egypt, Guyana, India, Mexico, Pakistan, and Sudan, using a convenience sampling technique, an online survey comprising demographic details, information regarding COVID-19, the Pittsburgh Sleep Quality Index (PSQI), and the Internet Addiction Test (IAT). Results In total, 2749 participants completed the questionnaire. Of the total, 67.6% scored above 30 in the IAT, suggesting the presence of an Internet addiction, and 73.5% scored equal and above 5 in the PSQI, suggesting poor sleep quality. Internet addiction was found to be significant predictors of poor sleep quality, causing 13.2% of the variance in poor sleep quality. Participants who reported COVID-19 related symptoms had disturbed sleep and higher internet addiction levels when compared with those who did not. Participants who reported a diagnosis of COVID-19 reported poor sleep quality. Those living with a COVID-19 diagnosed patient reported higher internet addiction and worse sleep quality compared with those who did not have any COVID-19 patients in their surroundings. Conclusion The results of this study suggest that internet addiction and poor sleep quality are two issues that require addressing amongst medical students. Medical training institutions should do their best to minimize their negative impact, particularly during the current COVID-19 pandemic.

Published
2021
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38. Family structure and substance use in 6,178 American Indian youth: a cross-sectional study.

Author

SHAH, J., SHAH, A., EL-SAKKA, A. A., KANDIL, O. A., SHEHATA, M. A., and SHOIB, S.

Abstract

OBJECTIVE: Adolescents from single-parent families are at significantly higher risk of substance use compared to those from mother-father families. More than half of American Indian (AI) children live in single-parent families, the second highest percentage among all groups. Given the paucity of research pertaining to the role of family structure and substance use in the AI population, we sought to examine this relationship. MATERIALS AND METHODS: Data from this study were obtained from the Substance Use Among American Indian Youth: Epidemiology and Etiology, [US], 2015-2020 study. Response variables of interest included age at first substance use, number of substances used, ever-use of substance, and substance use type (i.e., alcohol, cigarette, marijuana, etc.). RESULTS: Living in a father-only or mother-only setting showed a similar pattern of drug use. There was a significant increase in the risk of cigarette, alcohol and marijuana use. For cigarettes, the odds ratio was (OR = 2.60, 95% CI 1.80-3.75) in father-only setting compared to (OR = 1.42, 95% CI 1.13-1.78) for mother only setting. Alcohol use showed (OR = 1.72, 95% CI 1.19-2.50 and OR = 1.40, 95% CI 1.12-1.74) for father-only and mother-only respectively and marijuana use showed (OR = 1.59, 95% CI 1.10-2.30 and OR = 1.54, 95% CI -1.24-1.92) for father-only and mother-only respectively. CONCLUSIONS: Disturbed family structure is associated with increased risk of substance use among AI youth. This indicates the importance and need for policy and community level interventions to reduce youth substance exposure. [ABSTRACT FROM AUTHOR]

Published
2022

40. Tools to study and target the Siglec-sialic acid axis in cancer

Author

Cijo George Vazhappilly, Heinz Läubli, Rachel Matar, Kunio Kawanishi, Maxime Merheb, and Shoib S. Siddiqui

Subjects
0301 basic medicine, medicine.drug_class, medicine.medical_treatment, Neuraminidase, Monoclonal antibody, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cancer immunotherapy, Neoplasms, medicine, Humans, Tyrosine, Molecular Biology, Sialic Acid Binding Immunoglobulin-like Lectins, Innate immune system, SIGLEC, Cell Biology, respiratory system, Fusion protein, N-Acetylneuraminic Acid, Sialic acid, Cell biology, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Cancer cell
Abstract

Siglecs are widely expressed on leukocytes and bind to ubiquitously presented glycans containing sialic acids (sialoglycans). Most Siglecs carry an immunoreceptor tyrosine-based inhibition motif (ITIM) and elicit an inhibitory intracellular signal upon ligand binding. A few Siglec receptors can, however, recruit an immunoreceptor tyrosine-based activation motif (ITAM)-containing factors, which activate cells. The role of hypersialylation (the enhanced expression of sialolglycans) - in cancer progression has recently been explored. Mechanistic studies have shown that hypersialylation on cancer cells can engage inhibitory Siglecs on the surface of innate immune cells and induce immunosuppression. These recent studies strongly suggest that the Siglec-sialic acid axis can act as a potential target for cancer immunotherapy. Moreover, the use of new tools and techniques are facilitating these studies. In this review we summarise techniques used to study Siglecs, including different mouse models, monoclonal antibodies, Siglec fusion proteins and sialoglycan arrays. Furthermore, we discuss the recent major developments in the study of Siglecs in cancer immunosuppression, tools and techniques used in targeting the Siglec-sialic acid axis and the possibility of clinical intervention.

Published
2020

41. Human-specific polymorphic pseudogenization of

Author

Shoib S, Siddiqui, Michael, Vaill, Raymond, Do, Naazneen, Khan, Andrea L, Verhagen, Wu, Zhang, Heinz-Josef, Lenz, Teresa L, Johnson-Pais, Robin J, Leach, Gary, Fraser, Charles, Wang, Gen-Sheng, Feng, Nissi, Varki, and Ajit, Varki

Subjects
advanced carcinoma, dot blot, SIGLEC12, immunohistochemistry, respiratory system, pseudogenization, Research Articles, Research Article
Abstract

Compared with our closest living evolutionary cousins, humans appear unusually prone to develop carcinomas (cancers arising from epithelia). The SIGLEC12 gene, which encodes the Siglec‐XII protein expressed on epithelial cells, has several uniquely human features: a fixed homozygous missense mutation inactivating its natural ligand recognition property; a polymorphic frameshift mutation eliminating full‐length protein expression in ~60%–70% of worldwide human populations; and, genomic features suggesting a negative selective sweep favoring the pseudogene state. Despite the loss of canonical sialic acid binding, Siglec‐XII still recruits Shp2 and accelerates tumor growth in a mouse model. We hypothesized that dysfunctional Siglec‐XII facilitates human carcinoma progression, correlating with known tumorigenic signatures of Shp2‐dependent cancers. Immunohistochemistry was used to detect Siglec‐XII expression on tissue microarrays. PC‐3 prostate cancer cells were transfected with Siglec‐XII and transcription of genes enriched with Siglec‐XII was determined. Genomic SIGLEC12 status was determined for four different cancer cohorts. Finally, a dot blot analysis of human urinary epithelial cells was established to determine the Siglec‐XII expressors versus non‐expressors. Forced expression in a SIGLEC12 null carcinoma cell line enriched transcription of genes associated with cancer progression. While Siglec‐XII was detected as expected in ~30%–40% of normal epithelia, ~80% of advanced carcinomas showed strong expression. Notably, >80% of late‐stage colorectal cancers had a functional SIGLEC12 allele, correlating with overall increased mortality. Thus, advanced carcinomas are much more likely to occur in individuals whose genomes have an intact SIGLEC12 gene, likely because the encoded Siglec‐XII protein recruits Shp2‐related oncogenic pathways. The finding has prognostic, diagnostic, and therapeutic implications.

Published
2020

42. Acidosis, Zinc and HMGB1 in Sepsis: A Common Connection Involving Sialoglycan Recognition

Author

Leonard C. Harrison, Xi Chen, Shoib S. Siddiqui, Xiaoxiao Zhang, Venkatasubramaniam Sundaramurthy, Hai Yu, Aniruddha Sasmal, Ajit Varki, Ding Xu, Miaomiao Li, Chirag Dhar, and Esther Bandala-Sanchez

Subjects
Chemistry, chemistry.chemical_element, chemical and pharmacologic phenomena, Zinc, medicine.disease, Lactic acid, Proinflammatory cytokine, Sepsis, chemistry.chemical_compound, Biochemistry, Lactic acidosis, medicine, Sialoglycoproteins, medicine.symptom, Whole blood, Acidosis
Abstract

Blood pH is tightly regulated between 7.35-7.45, with values below 7.3 during sepsis being associated with lactic acidosis, low serum zinc, and release of proinflammatory HMGB1 from activated and/or necrotic cells. Using an ex vivo whole blood system to model lactic acidosis, we show that while HMGB1 does not engage leukocyte receptors at physiological pH, lowering pH with lactic acid facilitates binding. At normal pH, micromolar zinc supports plasma sialoglycoprotein binding by HMGB1, which is markedly reduced when pH is adjusted with lactic acid to sepsis levels. Glycan array studies confirmed zinc and pH-dependent HMGB1 binding to sialoglycans typical of plasma glycoproteins. Thus, proinflammatory effects of HMGB1 are suppressed via plasma sialoglycoproteins until drops in pH and zinc release HMGB1 to trigger downstream immune activation.Significance StatementHMGB1 sequestered by plasma sialoglycoproteins at physiological pH is released when pH and zinc concentrations fall in sepsis.

Published
2020

43. Dietary Flavonoids in p53-Mediated Immune Dysfunctions Linking to Cancer Prevention

Author

Cijo George Vazhappilly, Shoib S. Siddiqui, H.P. Vasantha Rupasinghe, and Sofia Rahman

Subjects
p53, medicine.medical_treatment, Medicine (miscellaneous), Inflammation, Review, Biology, medicine.disease_cause, Major histocompatibility complex, General Biochemistry, Genetics and Molecular Biology, Immune system, Cancer immunotherapy, medicine, lcsh:QH301-705.5, Cancer prevention, cancer prevention, anti-oxidant, Nrf2 pathway, Cancer, medicine.disease, KEAP1, lcsh:Biology (General), inflammation, flavonoids, biology.protein, Cancer research, medicine.symptom, Carcinogenesis
Abstract

The p53 protein plays a central role in mediating immune functioning and determines the fate of the cells. Its role as a tumor suppressor, and in transcriptional regulation and cytokine activity under stress conditions, is well defined. The wild type (WT) p53 functions as a guardian for the genome, while the mutant p53 has oncogenic roles. One of the ways that p53 combats carcinogenesis is by reducing inflammation. WT p53 functions as an anti-inflammatory molecule via cross-talk activity with multiple immunological pathways, such as the major histocompatibility complex I (MHCI) associated pathway, toll-like receptors (TLRs), and immune checkpoints. Due to the multifarious roles of p53 in cancer, it is a potent target for cancer immunotherapy. Plant flavonoids have been gaining recognition over the last two decades to use as a potential therapeutic regimen in ameliorating diseases. Recent studies have shown the ability of flavonoids to suppress chronic inflammation, specifically by modulating p53 responses. Further, the anti-oxidant Keap1/Nrf2/ARE pathway could play a crucial role in mitigating oxidative stress, leading to a reduction of chronic inflammation linked to the prevention of cancer. This review aims to discuss the pharmacological properties of plant flavonoids in response to various oxidative stresses and immune dysfunctions and analyzes the cross-talk between flavonoid-rich dietary intake for potential disease prevention.

Published
2020

47. Human‐specific polymorphic pseudogenization of SIGLEC12 protects against advanced cancer progression

Author

Siddiqui, Shoib S, primary, Vaill, Michael, additional, Do, Raymond, additional, Khan, Naazneen, additional, Verhagen, Andrea L, additional, Zhang, Wu, additional, Lenz, Heinz‐Josef, additional, Johnson‐Pais, Teresa L, additional, Leach, Robin J, additional, Fraser, Gary, additional, Wang, Charles, additional, Feng, Gen‐Sheng, additional, Varki, Nissi, additional, and Varki, Ajit, additional

Published
2020
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49. Siglecs in Brain Function and Neurological Disorders

Author

Hussain Al Zouabi, Cijo George Vazhappilly, Rachel Matar, John Marton, Maxime Merheb, Syed Azharuddin Shamsuddin, Rawad Hodeify, and Shoib S. Siddiqui

Subjects
Nervous system, Sialic Acid Binding Ig-like Lectin 2, brain, Sialic Acid Binding Ig-like Lectin 3, microglia, Review, Biology, multiple sclerosis, Mice, chemistry.chemical_compound, Immune system, Antigens, CD, ITAM, Sialoadhesin, medicine, Animals, Humans, neurological disorder, lcsh:QH301-705.5, Neuroinflammation, Sialic Acid Binding Immunoglobulin-like Lectins, Microglia, ganglioside, CD22, General Medicine, respiratory system, ITIM, N-Acetylneuraminic Acid, Sialic acid, Myelin-Associated Glycoprotein, myelin, medicine.anatomical_structure, chemistry, Siglecs, lcsh:Biology (General), sialic acid, Nervous System Diseases, Neuroscience, Alzheimer’s disease, Function (biology)
Abstract

Siglecs (Sialic acid-binding immunoglobulin-type lectins) are a I-type lectin that typically binds sialic acid. Siglecs are predominantly expressed in immune cells and generate activating or inhibitory signals. They are also shown to be expressed on the surface of cells in the nervous system and have been shown to play central roles in neuroinflammation. There has been a plethora of reviews outlining the studies pertaining to Siglecs in immune cells. However, this review aims to compile the articles on the role of Siglecs in brain function and neurological disorders. In humans, the most abundant Siglecs are CD33 (Siglec-3), Siglec-4 (myelin-associated glycoprotein/MAG), and Siglec-11, Whereas in mice the most abundant are Siglec-1 (sialoadhesin), Siglec-2 (CD22), Siglec-E, Siglec-F, and Siglec-H. This review is divided into three parts. Firstly, we discuss the general biological aspects of Siglecs that are expressed in nervous tissue. Secondly, we discuss about the role of Siglecs in brain function and molecular mechanism for their function. Finally, we collate the available information on Siglecs and neurological disorders. It is intriguing to study this family of proteins in neurological disorders because they carry immunoinhibitory and immunoactivating motifs that can be vital in neuroinflammation.

Published
2019

50. Dual actions of group B

Author

Satoshi, Uchiyama, Josh, Sun, Kyoko, Fukahori, Nao, Ando, Mengyou, Wu, Flavio, Schwarz, Shoib S, Siddiqui, Ajit, Varki, Jamey D, Marth, and Victor, Nizet

Subjects
Adult, Blood Platelets, Male, Mice, Knockout, Sialic Acid Binding Immunoglobulin-like Lectins, Blood Bactericidal Activity, Virulence Factors, Biological Sciences, Glycocalyx, Platelet Activation, N-Acetylneuraminic Acid, Streptococcus agalactiae, Antigens, Differentiation, B-Lymphocyte, Mice, Antigens, CD, Streptococcal Infections, bacteria, Animals, Humans, Female, Bacterial Capsules
Abstract

Circulating platelets have important functions in thrombosis and in modulating immune and inflammatory responses. However, the role of platelets in innate immunity to bacterial infection is largely unexplored. While human platelets rapidly kill Staphylococcus aureus, we found the neonatal pathogen group B Streptococcus (GBS) to be remarkably resistant to platelet killing. GBS possesses a capsule polysaccharide (CPS) with terminal α2,3-linked sialic acid (Sia) residues that mimic a common epitope present on the human cell surface glycocalyx. A GBS mutant deficient in CPS Sia was more efficiently killed by human platelets, thrombin-activated platelet releasate, and synthetic platelet-associated antimicrobial peptides. GBS Sia is known to bind inhibitory Sia-recognizing Ig superfamily lectins (Siglecs) to block neutrophil and macrophage activation. We show that human platelets also express high levels of inhibitory Siglec-9 on their surface, and that GBS can engage this receptor in a Sia-dependent manner to suppress platelet activation. In a mouse i.v. infection model, antibody-mediated platelet depletion increased susceptibility to platelet-sensitive S. aureus but did not alter susceptibility to platelet-resistant GBS. Elimination of murine inhibitory Siglec-E partially reversed platelet suppression in response to GBS infection. We conclude that GBS Sia has dual roles in counteracting platelet antimicrobial immunity: conferring intrinsic resistance to platelet-derived antimicrobial components and inhibiting platelet activation through engagement of inhibitory Siglecs. We report a bacterial virulence factor for evasion of platelet-mediated innate immunity.

Published
2019

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