Genome‐wide association study of psoriasis in an Egyptian population

Bejaoui, Yosra; Witte, Mareike; Abdelhady, Mohamed; El-Darouti, Mohammad Ali; Abdallah, Nermeen; Elghzaly, Ashraf Antar; Tawhid, Ziyad; Gaballah, Mohammad A.; Busch, Hauke; Munz, Matthias; Wendorff, Mareike; Ellinghaus, Eva; Franke, André; Ibrahim, Saleh M.

doi:10.1111/exd.13926

Cited by 14 publications

(8 citation statements)

References 23 publications

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“…We investigated the impact of Egyptian ancestry on disease risk assessment by integrating Egyptian variant data with the GWAS catalog 50 , a curated database of GWAS. According to the GWAS catalog, most published GWAS are performed on Europeans 24 , and only a single study has been performed on Egyptians 51 (by one of the co-authors). Furthermore, only 2% of individuals included in GWAS are of African ancestry 24 .…”

Section: Resultsmentioning

confidence: 99%

An integrated personal and population-based Egyptian genome reference

Wohlers¹,

Künstner²,

Munz³

et al. 2020

Nat Commun

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A small number of de novo assembled human genomes have been reported to date, and few have been complemented with population-based genetic variation, which is particularly important for North Africa, a region underrepresented in current genome-wide references. Here, we combine long- and short-read whole-genome sequencing data with recent assembly approaches into a de novo assembly of an Egyptian genome. The assembly demonstrates well-balanced quality metrics and is complemented with variant phasing via linked reads into haploblocks, which we associate with gene expression changes in blood. To construct an Egyptian genome reference, we identify genome-wide genetic variation within a cohort of 110 Egyptian individuals. We show that differences in allele frequencies and linkage disequilibrium between Egyptians and Europeans may compromise the transferability of European ancestry-based genetic disease risk and polygenic scores, substantiating the need for multi-ethnic genome references. Thus, the Egyptian genome reference will be a valuable resource for precision medicine.

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Section: Resultsmentioning

confidence: 99%

An integrated personal and population-based Egyptian genome reference

Wohlers¹,

Künstner²,

Munz³

et al. 2020

Nat Commun

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“… 38 The literature supports some differences between familial and sporadic cases of psoriasis. 39 Differences in the strength of the association between the mutant gene and family history have been reported for the MHC, including a strong association of HLA-C*06 and HLA-B*27 with psoriasis.…”

Section: Discussionmentioning

confidence: 99%

Variants in PRKCE and KLC1, Potential Regulators of Type I Psoriasis

Xing¹,

Wang²,

Zhao³

et al. 2022

CCID

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Purpose Psoriasis is a multifactorial disease with a complex genetic predisposition. The pathophysiology of psoriasis is associated with genetic variants. To better characterize gene variants in psoriasis and identify the relationship between clinical characteristics and variant genes in its pathogenesis. Patients and Methods DNA was extracted and purified from eight pairs of monozygotic twins with psoriasis discordance and 282 type I psoriasis patients. Thirteen variable genes were amplified and sequenced using the Sanger method after whole genome sequencing. Results Thirteen genes were found to be variable in eight pairs of monozygotic twins with psoriasis discordance. Among the 13 genes, the variant frequencies of protein kinase C epsilon (PRKCE) (c.240T>C, 35.9% vs 47.7%, P < 0.05) and kinesin light chain 1 (KLC1) (c.216A>G, 2.9% vs 98.1%, P< 0.01) were significantly lower in psoriasis than in normal Asian individuals. Additionally, we found considerable differences in the relationship between variants in genes CADM2 , JPH2 , SPTLC3 and clinical characteristics stratified by medical history and family history. Moreover, the variants in MEGF6 (39.52% vs 22.50%, χ 2 =3.83, p < 0.05) showed a stronger association with the mild group (PASI ≤10) than the heavy group. Conclusion Our results provide a comprehensive correlation analysis of regulatory genes that are regulated in psoriasis. This integrated analysis offers novel insight into the pathogenic mechanisms involved in psoriasis.

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“…In contrast, type 2associated cells, including T H 2 cells, eosinophils, basophils and ILC2 can increase during AD. GWAS analysis (publicly available databases: GWAS database, https://www.ebi.ac.uk/gwas/; GWAS Central, https://www.gwascentral.org/; accessed 15.11.2021; filtered for psoriasis and atopic eczema traits) of the most common SNPs associated with psoriasis (Pso) and atopic dermatitis (AD) are summarised in the Venn diagram rs6913137, rs2853950, rs3130573, rs7756521, rs9263717, rs2233959, rs2524096, rs12199223, rs1265078, rs2249742, rs2853961, and many more [191,192] TNFAIP3 rs582757, rs610604, rs6933987, rs643177 [181,[193][194][195][196] NFKB1A rs8016947 [193,196] IL36RN rs387906914, rs397514629 [75,197,198] LCE3B rs4845454, rs11205044, rs1581803 [64,199,200] LCE3D rs4085613, rs4112788, rs6677595 [193,194,201] AD and psoriasis HLA-A/B AD: rs148203517, rs4713555, rs28752924, rs28383323, rs200291258, rs9405068, rs4713555, rs2251396; Pso: rs4406273, rs2523619, rs17728338, rs75851973, rs76956521, rs1960278, rs12212594, rs4959062, rs4349859, rs10484554 [64,80,172,173,181,191,193,196,202] CARD14 AD: rs535171797; Pso: rs11652075 [193,203] IL12B AD: rs3212227, rs393548, rs436857; Pso: rs2082412, rs3212227, rs3213094, rs2546890, rs12188300, rs12188300, rs6887695 [78,[193][194][195][204][205][206] IL13 AD: rs848, rs1295686, rs847, rs1295685, rs20541, rs12188917; Pso: rs20541, rs1295685, rs847…”

Section: F I G U R E 1 Schematic Representation Of Skin and Underlyin...mentioning

confidence: 99%

Break on through: The role of innate immunity and barrier defence in atopic dermatitis and psoriasis

Hawerkamp

Fahy

Fallon

et al. 2022

Skin Health and Disease

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The human skin can be affected by a multitude of diseases including inflammatory conditions such as atopic dermatitis and psoriasis. Here, we describe how skin barrier integrity and immunity become dysregulated during these two most common inflammatory skin conditions. We summarise recent advances made in the field of the skin innate immune system and its interaction with adaptive immunity. We review gene variants associated with atopic dermatitis and psoriasis that affect innate immune mechanisms and skin barrier integrity. Finally, we discuss how current and future therapies may affect innate immune responses and skin barrier integrity in a generalized or more targeted approach in order to ameliorate disease in patients.

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Genome‐wide association study of psoriasis in an Egyptian population

Cited by 14 publications

References 23 publications

An integrated personal and population-based Egyptian genome reference

An integrated personal and population-based Egyptian genome reference

Variants in PRKCE and KLC1, Potential Regulators of Type I Psoriasis

Break on through: The role of innate immunity and barrier defence in atopic dermatitis and psoriasis

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