Deciphering the role of a SINE-VNTR-Alu retrotransposon polymorphism as a biomarker of Parkinson’s disease progression

Fröhlich, Alexander; Pfaff, Abigail L.; Middlehurst, Ben; Hughes, Lauren S.; Bubb, Vivien J.; Quinn, John P.; Koks, Sulev

doi:10.1038/s41598-024-61753-5

Cited by 3 publications

References 58 publications

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Transposable element small and long RNAs in aging brains and implications in Huntington’s and Parkinson’s disease

Dayama,

Gupta,

Connizzo

et al. 2024

Preprint

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Transposable Elements (TEs) are implicated in aging and neurodegenerative disorders, but the impact of brain TE RNA dynamics on these phenomena is not fully understood. Therefore, we quantified TE RNA changes in aging post-mortem human and mouse brains and in the neurodegenerative disorders Huntington's Disease (HD) and Parkinson's Disease (PD). We tracked TE small RNAs (smRNAs) expression landscape to assess the relationship to the active processing from TE long RNAs (lnRNAs). Human brain transcriptomes from the BrainSpan Atlas displayed a significant shift of TE smRNA patterns at age 20 years, whereas aging mouse brains lacked any such marked change, despite clear shift in aging-associated mRNA levels. Human frontal cortex displayed pronounced sense TE smRNAs during aging with a negative relationship between the TE smRNAs and lnRNAs indicative of age associated regulatory effects. Our analysis revealed TE smRNAs dysregulation in HD, while PD showed a stronger impact on TE lnRNAs, potentially correlating with the early average age of death for HD relative to PD. Furthermore, TE-silencing factor TRIM28 was down-regulated only in aging human brains, possibly explaining the lack of substantial TE RNA changes in aging mouse brains. Our study suggests brain TE RNAs may serve as novel biomarkers of human brain aging and neurodegenerative disorders.

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Transposable element small and long RNAs in aging brains and implications in Huntington’s and Parkinson’s disease

Dayama,

Gupta,

Connizzo

et al. 2024

Preprint

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SVA Regulation of Transposable Element Clustered Transcription within the Major Histocompatibility Complex Genomic Class II Region of the Parkinson’s Progression Markers Initiative

Kulski,

Pfaff,

Koks

2024

Genes

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SINE-VNTR-Alu (SVA) retrotransposons can regulate expression quantitative trait loci (eQTL) of coding and noncoding genes including transposable elements (TEs) distributed throughout the human genome. Previously, we reported that expressed SVAs and human leucocyte antigen (HLA) class II genotypes on chromosome 6 were associated significantly with Parkinson’s disease (PD). Here, our aim was to follow-up our previous study and evaluate the SVA associations and their regulatory effects on the transcription of TEs within the HLA class II genomic region. We reanalyzed the transcriptome data of peripheral blood cells from the Parkinson’s Progression Markers Initiative (PPMI) for 1530 subjects for TE and gene RNAs with publicly available computing packages. Four structurally polymorphic SVAs regulate the transcription of 20 distinct clusters of 235 TE loci represented by LINES (37%), SINES (28%), LTR/ERVs (23%), and ancient transposon DNA elements (12%) that are located in close proximity to HLA genes. The transcribed TEs were mostly short length, with an average size of 389 nucleotides. The numbers, types and profiles of positive and negative regulation of TE transcription varied markedly between the four regulatory SVAs. The expressed SVA and TE RNAs in blood cells appear to be enhancer-like elements that are coordinated differentially in the regulation of HLA class II genes. Future work on the mechanisms underlying their regulation and potential impact is essential for elucidating their roles in normal cellular processes and disease pathogenesis.

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Вирусо-Эпигенетическая Гипотеза Этиопатогенеза Болезни Паркинсона

Мустафин

2024

Успехи Геронтологии

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Накопленные в научной литературе данные свидетельствуют о том, что болезнь Паркинсона иногда развивается после перенесенных инфекций, вызванных вирусами SARS-CoV-2, Западного Нила, Коксаки, Сент-Луиса, японского энцефалита В, гепатита В и С, гриппа А, ВИЧ, герпес-вирусами, флавивирусами. Нейроинвазивные вирусы Западного Нила и ВИЧ активируют экспрессию альфа-синуклеина, а вирусы гриппа А, SARS-CoV-2 и Коксаки В3 способствуют агрегации альфа-синуклеина, который обладает биофизическими характеристиками противовирусных пептидов и необходим для нейрональной экспрессии генов, стимулируемых интерфероном. Данные механизмы могут быть триггерами болезни Паркинсона, прогрессирование которой обусловлено вовлечением в процесс активированных под их влиянием ретроэлементов, стимулирующих интерфероновый ответ, экспрессию и агрегацию альфа-синуклеина в головном мозге. Идентифицировано непосредственное активирующее влияние описанных вирусных инфекций на ретроэлементы генома человека. Дополнительными факторами являются ассоциированные с болезнью Паркинсона старение и полиморфизмы, расположенные в межгенных, интронных и регуляторных областях, где локализуются последовательности транспозонов. Кроме того, определено влияние особенностей распределения ретроэлементов в геномах популяций людей на предрасположенность к болезни Паркинсона и роль транспозонов в моногенных формах заболевания. Эффектами патологически активированных при болезни Паркинсона ретроэлементов являются изменения экспрессии произошедших от них микроРНК, которые способствуют нарушению эпигенетической регуляции генов в головном мозге и прогрессированию патологии. Анализ научной литературы позволил описать снижение уровня 15 таких микроРНК, которые могут служить инструментами для таргетной терапии заболевания. Data accumulated in scientific literature indicate that Parkinson’s disease develops after infections caused by SARS-CoV-2, West Nile, Coxsackie, St. Louis viruses, Japanese encephalitis B, hepatitis B and C, influenza A, HIV, herpes viruses, flaviviruses. Neuroinvasive West Nile viruses and HIV activate expression of alpha-synuclein. Influenza A, SARS-CoV-2, and Coxsackie B3 viruses promote aggregation of alpha-synuclein, which has the biophysical characteristics of antiviral peptides and is required for neuronal interferon-stimulated gene expression. These mechanisms can be triggers of Parkinson’s disease, which progression is due to involvement of retroelements activated under their influence, stimulating the interferon response, expression and aggregation of alpha-synuclein in the brain. Direct activation of retroelements of the human genome by the described viral infections has been identified. Additional factors are aging and Parkinson’s disease-associated polymorphisms located in intergenic, intronic and regulatory regions where transposon sequences are localized. In addition, the influence of the distribution of retroelements in the genomes of human populations on susceptibility to Parkinson’s disease and the role of transposons in monogenic forms of the disease were determined. The effects of pathologically activated retroelements in Parkinson’s disease are changes in expression of microRNAs derived from them, which contribute to disruption of epigenetic regulation of genes in the brain and pathology progression. An analysis of the scientific literature made it possible to describe a decrease in the levels of 15 such microRNAs, which can serve as tools for targeted therapy of the disease.

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Deciphering the role of a SINE-VNTR-Alu retrotransposon polymorphism as a biomarker of Parkinson’s disease progression

Cited by 3 publications

References 58 publications

Transposable element small and long RNAs in aging brains and implications in Huntington’s and Parkinson’s disease

Transposable element small and long RNAs in aging brains and implications in Huntington’s and Parkinson’s disease

SVA Regulation of Transposable Element Clustered Transcription within the Major Histocompatibility Complex Genomic Class II Region of the Parkinson’s Progression Markers Initiative

Вирусо-Эпигенетическая Гипотеза Этиопатогенеза Болезни Паркинсона

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