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3. Fusing Peptide Epitopes for Advanced Multiplex Serological Testing for SARS-CoV-2 Antibody Detection

Author

Aldoukhi, Ali H., primary, Bilalis, Panayiotis, additional, Alhattab, Dana M., additional, Valle-Pérez, Alexander U., additional, Susapto, Hepi H., additional, Pérez-Pedroza, Rosario, additional, Backhoff-García, Emiliano, additional, Alsawaf, Sarah M., additional, Alshehri, Salwa, additional, Boshah, Hattan, additional, Alrashoudi, Abdulelah A., additional, Aljabr, Waleed A., additional, Alaamery, Manal, additional, Alrashed, May, additional, Hasanato, Rana M., additional, Farzan, Raed A., additional, Alsubki, Roua A., additional, Moretti, Manola, additional, Abedalthagafi, Malak S., additional, and Hauser, Charlotte A. E., additional

Published
2023
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4. Factors that influence a patient’s decision to engage in genetic research

Author

Almutairi, Amal, primary, Alqubaishi, Fatimah Abdulrahman, additional, Alsolm, Ebtehal A., additional, Binowayn, Albandari, additional, Almohammad, Rania, additional, Wani, Tariq, additional, Ababtain, Aljohara, additional, Alkadi, Udai, additional, Alrashed, May M., additional, Althagafi, Malak, additional, and Abu-Safieh, Leen, additional

Published
2023
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6. A unique investigation of thallium, tellurium, osmium, and other heavy metals in recurrent pregnancy loss: A novel approach

Author

Tabassum, Hajera, primary, Alrashed, May, additional, Malik, Abdul, additional, Alanazi, Samyah T., additional, Alenzi, Naif D., additional, Ali, Mir Naiman, additional, AlJaser, Feda S., additional, Altoum, Ghadah H., additional, Hijazy, Sereen M., additional, Alfadhli, Reem A., additional, Alrashoudi, Reem, additional, and Akhtar, Suhail, additional

Published
2022
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7. Isolated Congenital Anosmia: Case Report and Literature Review

Author

Alotaibi, Naif H., primary, Alrashed, May, additional, Alenezi, Mohammed K. D., additional, Abu-Safieh, Leen, additional, Almobarak, Abdulaziz A., additional, Baz, Batoul, additional, Farzan, Raed A., additional, Alsuhaibani, Mohanned S., additional, and Al-Alsheikh, Yazeed, additional

Published
2022
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8. Biomarker-Determined Nonylphenol Exposure and Associated Risks in Children of Thailand, Indonesia, and Saudi Arabia

Author

Ringbeck, Benedikt, primary, Bury, Daniel, additional, Lee, Inae, additional, Lee, Gowoon, additional, Alakeel, Raid, additional, Alrashed, May, additional, Tosepu, Ramadhan, additional, Jayadipraja, Erwin Azizi, additional, Tantrakarnapa, Kraichat, additional, Kliengchuay, Wissanupong, additional, Brüning, Thomas, additional, Choi, Kyungho, additional, and Koch, Holger M., additional

Published
2022
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9. Detection of Novel Biallelic Causative Variants in COL7A1 Gene by Whole-Exome Sequencing, Resulting in Congenital Recessive Dystrophic Epidermolysis Bullosa in Three Unrelated Families

Author

Fozia, Fozia, primary, Nazli, Rubina, additional, Alrashed, May Mohammed, additional, Ghneim, Hazem K., additional, Haq, Zia Ul, additional, Jabeen, Musarrat, additional, Alam Khan, Sher, additional, Ahmad, Ijaz, additional, Bourhia, Mohammed, additional, and Aboul-Soud, Mourad A. M., additional

Published
2022
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10. A unique investigation of thallium, tellurium, osmium, and other heavy metals in recurrent pregnancy loss: A novel approach.

Author

Tabassum, Hajera, Alrashed, May, Malik, Abdul, Alanazi, Samyah T., Alenzi, Naif D., Ali, Mir Naiman, AlJaser, Feda S., Altoum, Ghadah H., Hijazy, Sereen M., Alfadhli, Reem A., Alrashoudi, Reem, and Akhtar, Suhail

Subjects
*RECURRENT miscarriage, *OSMIUM, *HEAVY metals, *THALLIUM, *TELLURIUM, *OXIDANT status
Abstract

Objective: To study the impact of heavy metals especially tellurium, thallium, and osmium, in recurrent pregnancy loss (RPL) and to study their association with antioxidant status and DNA damage. Methods: This case–control study included women with RPL (n = 30) and healthy pregnant women as control (n = 30). Following blood collection, serum levels of thallium, tellurium, osmium, lead, mercury, and cadmium were estimated by inductively coupled plasma mass spectrophotometer. Results: Women with RPL exhibited significantly higher levels of heavy metals (P < 0.001) when compared with control women. Intriguingly, increased levels of serum thallium, tellurium, osmium, and lead were negatively correlated with total antioxidant status (P < 0.05). Further, the RPL group demonstrated strong positive correlation between heavy metals (thallium, tellurium, osmium, lead) and DNA damage (P < 0.05). No significant correlation between other heavy metals and markers of cellular damage was noted. Conclusion: Enhanced levels of heavy metals in women with RPL and correlation of thallium, tellurium, osmium, and lead with markers of cellular damage reflect the role of heavy metal poisoning, especially thallium, tellurium, and osmium, as potential risk factor in the etiology underlying recurrent miscarriage. Synopsis: Higher levels of thallium, tellurium, and osmium and subsequent cellular damage are indicative of heavy metal poisoning as potential risk factor underlying recurrent pregnancy loss. [ABSTRACT FROM AUTHOR]

Published
2023
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13. Urinary Concentrations of Major Phthalate and Alternative Plasticizer Metabolites in Children of Thailand, Indonesia, and Saudi Arabia, and Associated Risks

Author

Lee, Inae, primary, Pälmke, Claudia, additional, Ringbeck, Benedikt, additional, Ihn, Yunchul, additional, Gotthardt, Alexandra, additional, Lee, Gowoon, additional, Alakeel, Raid, additional, Alrashed, May, additional, Tosepu, Ramadhan, additional, Jayadipraja, Erwin Azizi, additional, Tantrakarnapa, Kraichat, additional, Kliengchuay, Wissanupong, additional, Kho, Younglim, additional, Koch, Holger M., additional, and Choi, Kyungho, additional

Published
2021
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15. Rare loss-of-function variants in type I IFN immunity genes are not associated with severe COVID-19

Author

Povysil, Gundula, primary, Butler-Laporte, Guillaume, additional, Shang, Ning, additional, Wang, Chen, additional, Khan, Atlas, additional, Alaamery, Manal, additional, Nakanishi, Tomoko, additional, Zhou, Sirui, additional, Forgetta, Vincenzo, additional, Eveleigh, Robert J.M., additional, Bourgey, Mathieu, additional, Aziz, Naveed, additional, Jones, Steven J.M., additional, Knoppers, Bartha, additional, Scherer, Stephen W., additional, Strug, Lisa J., additional, Lepage, Pierre, additional, Ragoussis, Jiannis, additional, Bourque, Guillaume, additional, Alghamdi, Jahad, additional, Aljawini, Nora, additional, Albes, Nour, additional, Al-Afghani, Hani M., additional, Alghamdi, Bader, additional, Almutairi, Mansour S., additional, Mahmoud, Ebrahim Sabri, additional, Abu-Safieh, Leen, additional, El Bardisy, Hadeel, additional, Harthi, Fawz S. Al, additional, Alshareef, Abdulraheem, additional, Suliman, Bandar Ali, additional, Alqahtani, Saleh A., additional, Almalik, Abdulaziz, additional, Alrashed, May M., additional, Massadeh, Salam, additional, Mooser, Vincent, additional, Lathrop, Mark, additional, Fawzy, Mohamed, additional, Arabi, Yaseen M., additional, Mbarek, Hamdi, additional, Saad, Chadi, additional, Al-Muftah, Wadha, additional, Jung, Junghyun, additional, Mangul, Serghei, additional, Badji, Radja, additional, Thani, Asma Al, additional, Ismail, Said I., additional, Gharavi, Ali G., additional, Abedalthagafi, Malak S., additional, Richards, J. Brent, additional, Goldstein, David B., additional, and Kiryluk, Krzysztof, additional

Published
2021
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18. Selenium Nanoparticles by Moderating Oxidative Stress Promote Differentiation of Mesenchymal Stem Cells to Osteoblasts

Author

Fatima,Sabiha, Alfrayh,Rawan, Alrashed,May, Alsobaie,Sarah, Ahmad,Rehan, Mahmood,Amer, Fatima,Sabiha, Alfrayh,Rawan, Alrashed,May, Alsobaie,Sarah, Ahmad,Rehan, and Mahmood,Amer

Abstract

Sabiha Fatima,1 Rawan Alfrayh,1 May Alrashed,2 Sarah Alsobaie,1 Rehan Ahmad,3 Amer Mahmood4 1Department of Clinical Laboratory Sciences, College of Applied Medical Sciences, King Saud University, Riyadh 11433, Saudi Arabia; 2Chair of Medical and Molecular Genetics Research, Department of Clinical Laboratory Sciences, College of Applied Medical Sciences, King Saud University, Riyadh 11433, Saudi Arabia; 3Colorectal Research Chair, Department of Surgery, King Saud University, College of Medicine, Riyadh 11472, Saudi Arabia; 4Stem Cell Unit, Department of Anatomy, College of Medicine, King Khalid University Hospital, King Saud University, Riyadh 11461, Kingdom of Saudi ArabiaCorrespondence: Sabiha FatimaDepartment of Clinical Laboratory Sciences, College of Applied Medical Sciences, King Saud University, Riyadh, Saudi ArabiaTel +966-11-8052621Fax +966-11-4693738Email sabmehdi@ksu.edu.saAmer MahmoodStem Cell Unit, Department of Anatomy, College of Medicine, King Saud University, Riyadh 11461, Kingdom of Saudi ArabiaTel +966-11-4679421Fax +966-11-4693738Email ammahmood@ksu.edu.saPurpose: Redox homeostasis plays an important role in the osteogenic differentiation of human mesenchymal stem cells (hMSCs) for bone engineering. Oxidative stress (OS) is believed to induce osteoporosis by changing bone homeostasis. Selenium nanoparticles (SeNPs), an antioxidant with pleiotropic pharmacological activity, prevent bone loss. However, the molecular mechanism underlying the osteogenic activity during hMSC–SeNP interaction is unclear.Methods: This study assessed the effects of different concentrations (25, 50, 100, and 300 ng/mL) of SeNPs on the cell viability and differentiation ability of human embryonic stem cell-derived hMSCs. In addition, we analyzed OS markers and their effect on mitogen-activated protein kinase (MAPK) and Forkhead box O3 (FOXO3) during osteogenesis.Results: SeNPs increased the cell viability of hMSCs and induced their differentiation toward an osteog

Published
2021

19. Landscape of somatic mutations in breast cancer: new opportunities for targeted therapies in Saudi Arabian patients

Author

Barakeh, Duna H., primary, Aljelaify, Rasha, additional, Bashawri, Yara, additional, Almutairi, Amal, additional, Alqubaishi, Fatimah, additional, Alnamnakani, Mohammed, additional, Almubarak, Latifa, additional, Al Naeem, Abdulrahman, additional, Almushawah, Fatema, additional, Alrashed, May, additional, and Abedalthagafi, Malak, additional

Published
2021
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22. Failure to replicate the association of rare loss-of-function variants in type I IFN immunity genes with severe COVID-19

Author

Povysil, Gundula, primary, Butler-Laporte, Guillaume, additional, Shang, Ning, additional, Weng, Chen, additional, Khan, Atlas, additional, Alaamery, Manal, additional, Nakanishi, Tomoko, additional, Zhou, Sirui, additional, Forgetta, Vincenzo, additional, Eveleigh, Robert, additional, Bourgey, Mathieu, additional, Aziz, Naveed, additional, Jones, Steven, additional, Knoppers, Bartha, additional, Scherer, Stephen, additional, Strug, Lisa, additional, Lepage, Pierre, additional, Ragoussis, Jiannis, additional, Bourque, Guillaume, additional, Alghamdi, Jahad, additional, Aljawini, Nora, additional, Albes, Nour, additional, Al-Afghani, Hani M., additional, Alghamdi, Bader, additional, Almutair, Mansour, additional, Mahmoud, Ebrahim Sabri, additional, Safie, Leen Abu, additional, Bardisy, Hadeel El, additional, Harthi, Fawz S. Al, additional, Alshareef, Abdulraheem, additional, Suliman, Bandar Ali, additional, Alqahtani, Saleh, additional, AlMalik, Abdulaziz, additional, Alrashed, May M., additional, Massadeh, Salam, additional, Mooser, Vincent, additional, Lathrop, Mark, additional, Arabi, Yaseen, additional, Mbarek, Hamdi, additional, Saad, Chadi, additional, Al-Muftah, Wadha, additional, Badji, Radja, additional, Thani, Asma Al, additional, Ismail, Said I., additional, Gharavi, Ali G., additional, Abedalthagafi, Malak S., additional, Richards, J Brent, additional, Goldstein, David B., additional, and Kiryluk, Krzysztof, additional

Published
2020
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25. MOLECULAR CHARACTERIZATION OF CARBAPENEMRESISTANCE GENES AMONG Pseudomonas aeruginosa AND Acinetobacter baumannii CLINICAL ISOLATES IN RIYADH.

Author

Jawhar, Wejdan Nasser Bin, AlRashed, May Mohammed, Somily, Ali Mohammed, and AlBarrag, Ahmed Mohammed

Subjects
*ACINETOBACTER baumannii, *PSEUDOMONAS aeruginosa infections, *PSEUDOMONAS aeruginosa, *MEDICAL microbiology, *GENES, *POLYMERASE chain reaction, *NOSOCOMIAL infections
Abstract

Background: Antimicrobial resistance in Gram-negative bacteria has been a serious threat and a global problem. Acinetobacter baumannii and Pseudomonas aeruginosa are considered a leading cause of nosocomial infections worldwide and in the KSA. Objectives: The present study aimed to recognize the genes encoding Carbapenem resistance in two different non-fermentative, Gramnegative, non-fastidious pathogens, such as P. aeruginosa and A. baumannii strains isolated from a tertiary care hospital in Riyadh, Saudi Arabia. Materials/Methods: A total of 115 clinical isolates (80 P. aeruginosa and 35 A. baumannii) were obtained from different body sources at the clinical microbiology laboratory at King Khalid University Hospital, Riyadh, Saudi Arabia, from June to December 2017. The identification and antibiotic susceptibility testing were made for all the isolates using conventional (E-test) and the automated Vitek®2 system. The antibiotic susceptibility profiles of the isolates were determined as recommended by the Clinical and Laboratory Standards Institute (CLSI 2014). Polymerase Chain Reaction (PCR) was carried out to detect 13 Carbapenemase genes (OXA-23, OXA-24, OXA-40, OXA-51, OXA-10, OXA-48, OXA-1, VIM, IMP, GIM, NDM, KPC, ISAba-1) with a total of 50 ng DNA template added to the 25µl reaction mixture. Sanger sequencing was carried out using BigDye® Terminator v3.1 Cycle Sequencing kit (in 20 µl reaction mixture) to confirm the amplification of the target sequence. Results: A total of 80 isolates of P. aeruginosa were tested for the presence of Carbapenemase genes by PCR amplification method. It was found that the most prevalent genes were OXA-23 (55%) followed by blaVIM (46%). The OXA-1 and blaGIM genes were present in 22% and 15% of the isolates, respectively. A. baumannii isolates, tested for the presence of Carbapenem-resistant genes, also showed a prevalence of OXA-23 gene with an occurrence of 85.7%. ISAba-1 insertion sequence was found in 27 isolates. Conclusion: The rates of carbapenem-resistant isolates conferring multiple resistance genes are worrisome, leaving the clinicians with limited treatment options with antimicrobial drugs. Therefore, proper use for infection control procedures and revision of the treatment and management strategies is undoubtedly required to reduce the spread of resistance genes in these pathogens. [ABSTRACT FROM AUTHOR]

Published
2020

26. Autozygome-guided exome sequencing in retinal dystrophy patients reveals pathogenetic mutations and novel candidate disease genes

Author

Abu-Safieh, Leen, primary, Alrashed, May, additional, Anazi, Shamsa, additional, Alkuraya, Hisham, additional, Khan, Arif O., additional, Al-Owain, Mohammed, additional, Al-Zahrani, Jawahir, additional, Al-Abdi, Lama, additional, Hashem, Mais, additional, Al-Tarimi, Salwa, additional, Sebai, Mohammed-Adeeb, additional, Shamia, Ahmed, additional, Ray-zack, Mohamed D., additional, Nassan, Malik, additional, Al-Hassnan, Zuhair N., additional, Rahbeeni, Zuhair, additional, Waheeb, Saad, additional, Alkharashi, Abdullah, additional, Abboud, Emad, additional, Al-Hazzaa, Selwa A.F., additional, and Alkuraya, Fowzan S., additional

Published
2012
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28. In search of triallelism in Bardet–Biedl syndrome

Author

Abu-Safieh, Leen, primary, Al-Anazi, Shamsa, additional, Al-Abdi, Lama, additional, Hashem, Mais, additional, Alkuraya, Hisham, additional, Alamr, Mushari, additional, Sirelkhatim, Mugtaba O, additional, Al-Hassnan, Zuhair, additional, Alkuraya, Basim, additional, Mohamed, Jawahir Y, additional, Al-Salem, Ahmad, additional, Alrashed, May, additional, Faqeih, Eissa, additional, Softah, Ameen, additional, Al-Hashem, Amal, additional, Wali, Sami, additional, Rahbeeni, Zuhair, additional, Alsayed, Moeen, additional, Khan, Arif O, additional, Al-Gazali, Lihadh, additional, Taschner, Peter EM, additional, Al-Hazzaa, Selwa, additional, and Alkuraya, Fowzan S, additional

Published
2012
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30. Autozygome-guided exome sequencing in retinal dystrophy patients reveals pathogenetic mutations and novel candidate disease genes.

Author

Abu-Safieh, Leen, Alrashed, May, Anazi, Shamsa, Alkuraya, Hisham, Khan, Arif O., Al-Owain, Mohammed, Al-Zahrani, Jawahir, Al-Abdi, Lama, Hashem, Mais, Al-Tarimi, Salwa, Sebai, Mohammed-Adeeb, Shamia, Ahmed, Ray-zack, Mohamed D., Nassan, Malik, Al-Hassnan, Zuhair N., Rahbeeni, Zuhair, Waheeb, Saad, Alkharashi, Abdullah, Abboud, Emad, and Al-Hazzaa, Selwa A. F.

Subjects
*RETINAL degeneration, *PHOTORECEPTORS, *BLINDNESS, *ETIOLOGY of diseases, *MEDICAL genetics, *GENOMICS
Abstract

Retinal dystrophy (RD) is a heterogeneous group of hereditary diseases caused by loss of photoreceptor function and contributes significantly to the etiology of blindness globally but especially in the industrialized world. The extreme locus and allelic heterogeneity of these disorders poses a major diagnostic challenge and often impedes the ability to provide a molecular diagnosis that can inform counseling and gene-specific treatment strategies. In a large cohort of nearly 150 RD families, we used genomic approaches in the form of autozygome-guided mutation analysis and exome sequencing to identify the likely causative genetic lesion in the majority of cases. Additionally, our study revealed six novel candidate disease genes (C21orf2, EMC1, KIAA1549, GPR125, ACBD5, and DTHD1), two of which (ACBD5 and DTHD1) were observed in the context of syndromic forms of RD that are described for the first time. [ABSTRACT FROM AUTHOR]

Published
2013
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31. Deciphering the link: A cutting‐edge exploration of the intriguing connection between recurrent pregnancy loss and rare earth elements—Lutetium, praseodymium, samarium, dysprosium, and cerium.

Author

Alrashoudi, Reem Hamoud, Tabassum, Hajera, Fatima, Sabiha, Abudawood, Manal, Alrashed, May, Alsaigh, Sara Mohammed, Siddiqi, Nikhat J., and AlSheikh, Yazeed A.

Subjects
*RARE earth metals, *OXIDANT status, *PREGNANT women, *LUTETIUM, *CERIUM
Abstract

Objective Methods Results Conclusion To evaluate the levels of serum rare earth elements (REEs): lutetium [Lu], praseodymium [Pr], samarium [Sm], dysprosium [Dy], and cerium [Ce] in pregnant women with recurrent pregnancy loss (RPL) and evaluate their relationship with total antioxidant capacity (TAC) and 8‐hydroxy‐2′‐deoxyguanosine (8‐OHdG), a marker of DNA damage.A case‐controlled study was conducted on a cohort of 60 female participants, with first‐trimester healthy pregnant women as the control group and pregnant women with a history of consecutive abortions as the recurrent pregnancy loss (RPL) group. Following blood collection, serum concentrations of Lu, Pr, Sm, Dy, and Ce were measured using an inductively coupled plasma mass spectrophotometer (ICP‐MS). Oxidative stress and DNA damage were evaluated through TAC and DNA damage marker (8‐OHdG).Serum levels of Lu, Pr, Sm, Dy, and Ce were higher in women with RPL compared with control (P < 0.001). Intriguingly, a strong significant negative correlation was observed between TAC and REEs (P < 0.05). Lu, Dy, and Ce demonstrated a significant positive correlation with increased DNA damage in the RPL group (P < 0.05). Contrary, there was no evidence of a correlation between 8‐OHdG and Pr and Sm.The study highlights a potential association between Lu, Sm, Dy, and Ce and an increased risk of RPL, highlighting REE‐induced toxicity as a major risk factor for RPL. The outcome of the study is to advance our understanding of the interplay between rare earth elements and RPL, with potential implications for reproductive medicine, environmental health, and the development of preventive strategies for individuals at risk of RPL. [ABSTRACT FROM AUTHOR]

Published
2024
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32. Differential expression of miR-130a-3p modulate ovarian epithelial carcinoma (OEC) cell development and could be a biomarker for OEC.

Author

Alrashed, May Mohammed, Ahmad, Mohammad, Yongmei, Wei, and Xiuyeng, Wang

Subjects
*BIOMARKERS, *OVERALL survival, *SURVIVAL rate, *CELL cycle, *CELL proliferation, *OVARIAN epithelial cancer, *LYMPHATIC metastasis
Abstract

• MicroRNAs (miRNAs) play a key role in controlling ovarian epithelial metastasis. • Study find miR-130a-3p expressions are lower in neighboring normal tissues. • MiR-130a-3p over-expression prevents cell proliferation and cell cycle production in OEC. • MiR-130a-3p can be used as a biomarker of prognosis and a possible OEC treatment target. A lot of research investigations, conducted in the recent years, establishes that microRNAs (miRNAs) have an important role in keeping both growth and metastasis of Ovarian Epithelial Carcinoma (OEC) under control. However, the clinical and functional role of miR-130a-3p in OEC is yet to be explored. Through quantitative reaction i.e., qRT-PCR, the expression of miR-130a-3p was assessed in tissues and cell lines of OEC patients. This analysis determined the relationship between the expression of miR-130a-3p and its clinicopathology with the overall survival rate of OEC patients. The author made use of cell counting analysis (CCK8) and in vitro flow cytometry to understand the functional and biological impact of miR-130a-3p expression. In comparison with neighboring normal tissues, the expression of miR-130a-3p was found to be lower in 7 OEC samples. Few reasons are cited for this scenario i.e., low expression of miR-130a-3p, such as low overall OEC patient survival rate, incidence of FIGO and metastasis of lymph nodes. miR-130a-3p has been found as an independent candidate for predicting the prognosis of OEC patients, as per Multivariate Cox research. When miR-130a-3p is over-expressed, as per the enhanced mechanism, it prevents both cell proliferation and cell cycle production in OEC. The current study findings emphasize that miR-130a-3p can be leveraged as a biomarker of prognosis and possibly as a target in the treatment of OEC. [ABSTRACT FROM AUTHOR]

Published
2021
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33. A first update on mapping the human genetic architecture of COVID-19

Author

COVID-19 Host Genetics Initiative, Pathak, GA, Karjalainen, J, Stevens, C, Neale, BM, Daly, M, Ganna, A, Andrews, SJ, Kanai, M, Cordioli, M, Polimanti, R, Harerimana, N, Pirinen, M, Liao, RG, Chwialkowska, K, Trankiem, A, Balaconis, MK, Nguyen, H, Solomonson, M, Veerapen, K, Wolford, B, Roberts, G, Park, D, Ball, CA, Coignet, M, McCurdy, S, Knight, S, Partha, R, Rhead, B, Zhang, M, Berkowitz, N, Gaddis, M, Noto, K, Ruiz, L, Pavlovic, M, Hong, EL, Rand, K, Girshick, A, Guturu, H, Baltzell, AH, Niemi, MEK, Rahmouni, S, Guntz, J, Beguin, Y, Pigazzini, S, Nkambule, L, Georges, M, Moutschen, M, Misset, B, Darcis, G, Guiot, J, Azarzar, S, Gofflot, S, Claassen, S, Malaise, O, Huynen, P, Meuris, C, Thys, M, Jacques, J, Leonard, P, Frippiat, F, Giot, J-B, Sauvage, A-S, Frenckell, CV, Belhaj, Y, Lambermont, B, Nakanishi, T, Morrison, DR, Mooser, V, Richards, JB, Butler-Laporte, G, Forgetta, V, Li, R, Ghosh, B, Laurent, L, Belisle, A, Henry, D, Abdullah, T, Adeleye, O, Mamlouk, N, Kimchi, N, Afrasiabi, Z, Rezk, N, Vulesevic, B, Bouab, M, Guzman, C, Petitjean, L, Tselios, C, Xue, X, Afilalo, J, Afilalo, M, Oliveira, M, Brenner, B, Brassard, N, Durand, M, Schurr, E, Lepage, P, Ragoussis, J, Auld, D, Chassé, M, Kaufmann, DE, Lathrop, GM, Adra, D, Hayward, C, Glessner, JT, Shaw, DM, Campbell, A, Morris, M, Hakonarson, H, Porteous, DJ, Below, J, Richmond, A, Chang, X, Polikowski, H, Lauren, PE, Chen, H-H, Wanying, Z, Fawns-Ritchie, C, North, K, McCormick, JB, Glessner, JR, Gignoux, CR, Wicks, SJ, Crooks, K, Barnes, KC, Daya, M, Shortt, J, Rafaels, N, Chavan, S, Timmers, PRHJ, Wilson, JF, Tenesa, A, Kerr, SM, D’Mellow, K, Shahin, D, El-Sherbiny, YM, von Hohenstaufen, KA, Sobh, A, Eltoukhy, MM, Nkambul, L, Elhadidy, TA, Abd Elghafar, MS, El-Jawhari, JJ, Mohamed, AAS, Elnagdy, MH, Samir, A, Abdel-Aziz, M, Khafaga, WT, El-Lawaty, WM, Torky, MS, El-shanshory, MR, Yassen, AM, Hegazy, MAF, Okasha, K, Eid, MA, Moahmed, HS, Medina-Gomez, C, Ikram, MA, Uitterlinden, AG, Mägi, R, Milani, L, Metspalu, A, Laisk, T, Läll, K, Lepamets, M, Esko, T, Reimann, E, Naaber, P, Laane, E, Pesukova, J, Peterson, P, Kisand, K, Tabri, J, Allos, R, Hensen, K, Starkopf, J, Ringmets, I, Tamm, A, Kallaste, A, Alavere, H, Metsalu, K, Puusepp, M, Batini, C, Tobin, MD, Venn, LD, Lee, PH, Shrine, N, Williams, AT, Guyatt, AL, John, C, Packer, RJ, Ali, A, Free, RC, Wang, X, Wain, LV, Hollox, EJ, Bee, CE, Adams, EL, Palotie, A, Ripatti, S, Ruotsalainen, S, Kristiansson, K, Koskelainen, S, Perola, M, Donner, K, Kivinen, K, Kaunisto, M, Rivolta, C, Bochud, P-Y, Bibert, S, Boillat, N, Nussle, SG, Albrich, W, Quinodoz, M, Kamdar, D, Suh, N, Neofytos, D, Erard, V, Voide, C, Friolet, R, Vollenweider, P, Pagani, JL, Oddo, M, zu Bentrup, FM, Conen, A, Clerc, O, Marchetti, O, Guillet, A, Guyat-Jacques, C, Foucras, S, Rime, M, Chassot, J, Jaquet, M, Viollet, RM, Lannepoudenx, Y, Portopena, L, Bochud, PY, Desgranges, F, Filippidis, P, Guéry, B, Haefliger, D, Kampouri, EE, Manuel, O, Munting, A, 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Trivedi, Bhavi, Wright, John, Finer, Sarah, Akhtar, Shaheen, Anwar, Mohammad, Arciero, Elena, Ashraf, Samina, Breen, Gerome, Chung, Raymond, Curtis, Charles J., Chowdhury, Maharun, Colligan, Grainne, Deloukas, Pano, Durham, Ceri, Griffiths, Chri, Hurles, Matt, Hussain, Shapna, Islam, Kamrul, Khan, Ahsan, Khan, Amara, Lavery, Cath, Lee, Sang Hyuck, Lerner, Robin, MacArthur, Daniel, MacLaughlin, Bev, Martin, Hilary, Miah, Shefa, Newman, Bill, Safa, Nishat, Tahmasebi, Farah, Griffiths, Christopher J., Smith, Albert V., Boughton, Andrew P., Li, Kevin W., LeFaive, Jonathon, Annis, Aubrey, Niavarani, Ahmadreza, Aliannejad, Rasoul, Sharififard, Bahareh, Amirsavadkouhi, Ali, Naderpour, Zeinab, Tadi, Hengameh Ansari, Aleagha, Afshar Etemadi, Ahmadi, Saeideh, Moghaddam, Seyed Behrooz Mohseni, Adamsara, Alireza, Saeedi, Morteza, Abdollahi, Hamed, Hosseini, Abdolmajid, Chariyavilaskul, Pajaree, Jantarabenjakul, Watsamon, Hirankarn, Nattiya, Chamnanphon, Monpat, Suttichet, Thitima B., Shotelersuk, Vorasuk, Pongpanich, Monnat, Phokaew, Chureerat, Chetruengchai, Wanna, Putchareon, Opa, Torvorapanit, Pattama, Puthanakit, Thanyawee, Suchartlikitwong, Pintip, Nilaratanakul, Voraphoj, Sodsai, Pimpayao, Brumpton, Ben M., Hveem, Kristian, Willer, Cristen, Zhou, Wei, Rogne, Tormod, Solligard, Erik, Åsvold, Bjørn Olav, Franke, Lude, Boezen, Marike, Deelen, Patrick, Claringbould, Annique, Lopera, Esteban, Warmerdam, Robert, Vonk, Judith. M., van Blokland, Irene, Lanting, Pauline, Ori, Anil P. S., Feng, Yen-Chen Anne, Mercader, Josep, Weiss, Scott T., Karlson, Elizabeth W., Smoller, Jordan W., Murphy, Shawn N., Meigs, James B., Woolley, Ann E., Green, Robert C., Perez, Emma F., Zöllner, Sebastian, Wang, Jiongming, Beck, Andrew, Sloofman, Laura G., Ascolillo, Steven, Sebra, Robert P., Collins, Brett L., Levy, Te, Buxbaum, Joseph D., Sealfon, Stuart C., Jordan, Daniel M., Thompson, Ryan C., Gettler, Kyle, Chaudhary, Kumardeep, Belbin, Gillian M., Preuss, Michael, Hoggart, Clive, Choi, Sam, Underwood, Slayton J., Salib, Irene, Britvan, Bari, Keller, Katherine, Tang, Lara, Peruggia, Michael, Hiester, Liam L., Niblo, Kristi, Aksentijevich, Alexandra, Labkowsky, Alexander, Karp, Avromie, Zlatopolsky, Menachem, Zyndorf, Marissa, Charney, Alexander W., Beckmann, Noam D., Schadt, Eric E., Abul-Husn, Noura S., Cho, Judy H., Itan, Yuval, Kenny, Eimear E., Loos, Ruth J. F., Nadkarni, Girish N., Do, Ron, O’Reilly, Paul, Huckins, Laura M., Ferreira, Manuel A. R., Abecasis, Goncalo R., Leader, Joseph B., Cantor, Michael N., Justice, Anne E., Carey, Dave J., Chittoor, Geetha, Josyula, Navya Shilpa, Kosmicki, Jack A., Horowitz, Julie E., Baras, Ari, Gass, Matthew C., Yadav, Ashish, Mirshahi, Tooraj, Hottenga, Jouke Jan, Bartels, Meike, de geus, Eco E. J. C., Nivard, Michel M. G., Verma, Anurag, Ritchie, Marylyn D., Rader, Daniel, Li, Binglan, Verma, Shefali S., Lucas, Anastasia, Bradford, Yuki, Abedalthagafi, Malak, Alaamery, Manal, Alshareef, Abdulraheem, Sawaji, Mona, Massadeh, Salam, AlMalik, Abdulaziz, Alqahtani, Saleh, Baraka, Dona, Harthi, Fawz Al, Alsolm, Ebtehal, Safieh, Leen Abu, Alowayn, Albandary M., Alqubaishi, Fatimah, Mutairi, Amal Al, Mangul, Serghei, Almutairi, Mansour, Aljawini, Nora, Albesher, Nour, Arabi, Yaseen M., Mahmoud, Ebrahim S., Khattab, Amin K., Halawani, Roaa T., Alahmadey, Ziab Z., Albakri, Jehad K., Felemban, Walaa A., Suliman, Bandar A., Hasanato, Rana, Al-Awdah, Laila, Alghamdi, Jahad, AlZahrani, Deema, AlJohani, Sameera, Al-Afghani, Hani, AlDhawi, Nouf, AlBardis, Hadeel, Alkwai, Sarah, Alswailm, Moneera, Almalki, Faisal, Albeladi, Maha, Almohammed, Iman, Barhoush, Eman, Albader, Anoud, Alotaibi, Sara, Alghamdi, Bader, Jung, Junghyun, fawzy, Mohammad S., Alrashed, May, Zeberg, Hugo, Nkambul, Lindo, Frithiof, Robert, Hultström, Michael, Lipcsey, Miklo, Tardif, Nicola, Rooyackers, Olav, Grip, Jonathan, Maricic, Tomislav, Helgeland, Øyvind, Magnus, Per, Trogstad, Lill-Iren S., Lee, Yunsung, Harris, Jennifer R., Mangino, Massimo, Spector, Tim D., Emma, Duncan, Moutsianas, Louka, Caulfield, Mark J., Scott, Richard H., Kousathanas, Athanasio, Pasko, Dorota, Walker, Susan, Stuckey, Alex, Odhams, Christopher A., Rhodes, Daniel, Fowler, Tom, Rendon, Augusto, Chan, Georgia, Arumugam, Prabhu, Karczewski, Konrad J., Martin, Alicia R., Wilson, Daniel J., Spencer, Chris C. A., Crook, Derrick W., Wyllie, David H., O’Connell, Anne Marie, Atkinson, Elizabeth G., Tsuo, Kristin, Baya, Nikola, Turley, Patrick, Gupta, Rahul, Walters, Raymond K., Palmer, Duncan S., Sarma, Gopal, Cheng, Nathan, Lu, Wenhan, Churchhouse, Claire, Goldstein, Jacqueline I., King, Daniel, Seed, Cotton, Daly, Mark J., Finucane, Hilary, Bryant, Sam, Satterstrom, F. Kyle, Band, Gavin, Earle, Sarah G., Lin, Shang-Kuan, Arning, Nicola, Koelling, Nil, Armstrong, Jacob, Rudkin, Justine K., Callier, Shawneequa, Cusick, Caroline, Soranzo, Nicole, Zhao, Jing Hua, Danesh, John, Angelantonio, Emanuele Di, Butterworth, Adam S., Sun, Yan V., Huffman, Jennifer E., Cho, Kelly, O’Donnell, Christopher J., Tsao, Phil, Gaziano, J. Michael, Peloso, Gina, Ho, Yuk-Lam, Smieszek, Sandra P., Polymeropoulos, Christo, Polymeropoulos, Vasilio, Polymeropoulos, Mihael H., Przychodzen, Bartlomiej P., Fernandez-Cadenas, Israel, Planas, Anna M., Perez-Tur, Jordi, Llucià-Carol, Laia, Cullell, Natalia, Muiño, Elena, Cárcel-Márquez, Jara, DeDiego, Marta L., Iglesias, Lara Lloret, Soriano, Alex, Rico, Veronica, Agüero, Daiana, Bedini, Josep L., Lozano, Francisco, Domingo, Carlo, Robles, Veronica, Ruiz-Jaén, Francisca, Márquez, Leonardo, Gomez, Juan, Coto, Eliecer, Albaiceta, Guillermo M., García-Clemente, Marta, Dalmau, David, Arranz, Maria J., Dietl, Beatriz, Serra-Llovich, Alex, Soler, Pere, Colobrán, Roger, Martín-Nalda, Andrea, Martínez, Alba Parra, Bernardo, David, Rojo, Silvia, Fiz-López, Aida, Arribas, Elisa, de la Cal-Sabater, Paloma, Segura, Tomá, González-Villa, Esther, Serrano-Heras, Gemma, Martí-Fàbregas, Joan, Jiménez-Xarrié, Elena, de Felipe Mimbrera, Alicia, Masjuan, Jaime, García-Madrona, Sebastian, Domínguez-Mayoral, Anna, Villalonga, Joan Montaner, Menéndez-Valladares, Paloma, Chasman, Daniel I., Sesso, Howard D., Manson, JoAnn E., Buring, Julie E., Ridker, Paul M., Franco, Giulianini, Davis, Lea, Lee, Sulggi, Priest, Jame, Sankaran, Vijay G., van Heel, David, Biesecker, Le, Kerchberger, V. Eric, Baillie, J. Kenneth, APH - Personalized Medicine, APH - Health Behaviors & Chronic Diseases, Biological Psychology, APH - Mental Health, AMS - Sports, AMS - Ageing & Vitality, APH - Methodology, Mccurdy, Shannon, Mccormick, Joseph B., Macarthur, Daniel, Maclaughlin, Bev, Lefaive, Jonathon, Almalik, Abdulaziz, Alzahrani, Deema, Aljohani, Sameera, Aldhawi, Nouf, Albardis, Hadeel, Fawzy, Mohammad S., Dediego, Marta L., Stem Cell Aging Leukemia and Lymphoma (SALL), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Life Course Epidemiology (LCE), Groningen Research Institute for Asthma and COPD (GRIAC), University of Zurich, COVID-19 Host Genetics Initiative, Barcelona Supercomputing Center, COVID-19 Genetics Initiative, including authors, Institute for Molecular Medicine Finland, and Data Science Genetic Epidemiology Lab

Subjects
Informàtica::Aplicacions de la informàtica::Bioinformàtica [Àrees temàtiques de la UPC], Quantitative Trait Loci, MUC5B PROMOTER POLYMORPHISM, Genome-wide association studies, COVID-19 (Malaltia), UFSP13-7 Evolution in Action: From Genomes to Ecosystems, COVID-19 (Disease), Settore BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, SDG 3 - Good Health and Well-being, Humans, genetics, Genetic variation, Genomes, Medicinsk genetik, 1000 Multidisciplinary, Multidisciplinary, Chromosome Mapping, COVID-19, Human Genetics, 10124 Institute of Molecular Life Sciences, covid-19, 3121 General medicine, internal medicine and other clinical medicine, 570 Life sciences, biology, Medical Genetics
Abstract

Matters arising from: Mapping the human genetic architecture of COVID-19 Original Article published on 08 July 2021 https://www.nature.com/articles/s41586-021-03767-x The COVID-19 pandemic continues to pose a major public health threat, especially in countries with low vaccination rates. To better understand the biological underpinnings of SARS-CoV-2 infection and COVID-19 severity, we formed the COVID-19 Host Genetics Initiative1. Here we present a genome-wide association study meta-analysis of up to 125,584 cases and over 2.5 million control individuals across 60 studies from 25 countries, adding 11 genome-wide significant loci compared with those previously identified2. Genes at new loci, including SFTPD, MUC5B and ACE2, reveal compelling insights regarding disease susceptibility and severity. Here we present meta-analyses bringing together 60 studies from 25 countries (Fig. 1 and Supplementary Table 1) for three COVID-19-related phenotypes: (1) individuals critically ill with COVID-19 on the basis of requiring respiratory support in hospital or who died as a consequence of the disease (9,376 cases, of which 3,197 are new in this data release, and 1,776,645 control individuals); (2) individuals with moderate or severe COVID-19 defined as those hospitalized due to symptoms associated with the infection (25,027 cases, 11,386 new and 2,836,272 control individuals); and (3) all cases with reported SARS-CoV-2 infection regardless of symptoms (125,584 cases, 76,022 new and 2,575,347 control individuals). Most studies have reported results before the roll out of the COVID-19 vaccination campaign. An overview of the study design is provided in Supplementary Fig. 1. We found a total of 23 genome-wide significant loci (P

Published
2022

34. Failure to replicate the association of rare loss-of-function variants in type I IFN immunity genes with severe COVID-19.

Author

Povysil G, Butler-Laporte G, Shang N, Weng C, Khan A, Alaamery M, Nakanishi T, Zhou S, Forgetta V, Eveleigh R, Bourgey M, Aziz N, Jones S, Knoppers B, Scherer S, Strug L, Lepage P, Ragoussis J, Bourque G, Alghamdi J, Aljawini N, Albes N, Al-Afghani HM, Alghamdi B, Almutair M, Mahmoud ES, Safie LA, Bardisy HE, Al Harthi FS, Alshareef A, Suliman BA, Alqahtani S, AlMalik A, Alrashed MM, Massadeh S, Mooser V, Lathrop M, Arabi Y, Mbarek H, Saad C, Al-Muftah W, Badji R, Al Thani A, Ismail SI, Gharavi AG, Abedalthagafi MS, Richards JB, Goldstein DB, and Kiryluk K

Abstract

A recent report found that rare predicted loss-of-function (pLOF) variants across 13 candidate genes in TLR3- and IRF7-dependent type I IFN pathways explain up to 3.5% of severe COVID-19 cases. We performed whole-exome or whole-genome sequencing of 1,934 COVID-19 cases (713 with severe and 1,221 with mild disease) and 15,251 ancestry-matched population controls across four independent COVID-19 biobanks. We then tested if rare pLOF variants in these 13 genes were associated with severe COVID-19. We identified only one rare pLOF mutation across these genes amongst 713 cases with severe COVID-19 and observed no enrichment of pLOFs in severe cases compared to population controls or mild COVID-19 cases. We find no evidence of association of rare loss-of-function variants in the proposed 13 candidate genes with severe COVID-19 outcomes.

Published
2020
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