Your search keyword '"Lorna W. Harries"' showing total 157 results

1. Comprehensive analysis of alternative splicing across multiple transcriptomic cohorts reveals prognostic signatures in prostate cancer

Author

Zhuofan Mou, Jack Spencer, John S. McGrath, and Lorna W. Harries

Subjects

Alternative splicing, Microarray, RNA-seq, Prognosis, Prostate cancer, Medicine, Genetics, QH426-470

Abstract

Abstract Background Alternative splicing (AS) plays a crucial role in transcriptomic diversity and is a hallmark of cancer that profoundly influences the development and progression of prostate cancer (PCa), a prevalent and potentially life-limiting cancer among men. Accumulating evidence has highlighted the association between AS dysregulation and the onset and progression of PCa. However, a comprehensive and integrative analysis of AS profiles at the event level, utilising data from multiple high-throughput cohorts and evaluating the prognosis of PCa progression, remains lacking and calls for thorough exploration. Results We identified a differentially expressed retained intron event in ZWINT across three distinct cohorts, encompassing an original array-based dataset profiled by us previously and two RNA sequencing (RNA-seq) datasets. Subsequent in-depth analyses of these RNA-seq datasets revealed 141 altered events, of which 21 demonstrated a significant association with patients’ biochemical recurrence-free survival (BCRFS). We formulated an AS event-based prognostic signature, capturing six pivotal events in genes CYP4F12, NFATC4, PIGO, CYP3A5, ALS2CL, and FXYD3. This signature effectively differentiated high-risk patients diagnosed with PCa, who experienced shorter BCRFS, from their low-risk counterparts. Notably, the signature's predictive power surpassed traditional clinicopathological markers in forecasting 5-year BCRFS, demonstrating robust performance in both internal and external validation sets. Lastly, we constructed a novel nomogram that integrates patients’ Gleason scores with pathological tumour stages, demonstrating improved prognostication of BCRFS. Conclusions Prediction of clinical progression remains elusive in PCa. This research uncovers novel splicing events associated with BCRFS, augmenting existing prognostic tools, thus potentially refining clinical decision-making.

Published

2023

2. Repurposing Drugs for Senotherapeutic Effect: Potential Senomorphic Effects of Female Synthetic Hormones

Author

Laura R. Bramwell, Ryan Frankum, and Lorna W. Harries

Subjects

senescence, structure–function screen, synthetic hormone, sex differences, sex-specific, senomorphic, Cytology, QH573-671

Abstract

Repurposing previously approved drugs may fast track the route to the clinic for potential senotherapeutics and improves the inefficiency of the clinical drug development pipeline. We performed a repurposing screen of 240 clinically approved molecules in human primary dermal fibroblasts for their effects on CDKN2A expression. Molecules demonstrating effects on CDKN2A expression underwent secondary screening for senescence-associated beta galactosidase (SAB) activity, based on effect size, direction, and/or molecule identity. Selected molecules then underwent a more detailed assessment of senescence phenotypes including proliferation, apoptosis, DNA damage, senescence-associated secretory phenotype (SASP) expression, and regulators of alternative splicing. A selection of the molecules demonstrating effects on senescence were then used in a new bioinformatic structure–function screen to identify common structural motifs. In total, 90 molecules displayed altered CDKN2A expression at one or other dose, of which 15 also displayed effects on SAB positivity in primary human dermal fibroblasts. Of these, 3 were associated with increased SAB activity, and 11 with reduced activity. The female synthetic sex hormones—diethylstilboestrol, ethynyl estradiol and levonorgestrel—were all associated with a reduction in aspects of the senescence phenotype in male cells, with no effects visible in female cells. Finally, we identified that the 30 compounds that decreased CDKN2A activity the most had a common substructure linked to this function. Our results suggest that several drugs licensed for other indications may warrant exploration as future senotherapies, but that different donors and potentially different sexes may respond differently to senotherapeutic compounds. This underlines the importance of considering donor-related characteristics when designing drug screening platforms.

Published

2024

3. An evaluation of the role of miR-361-5p in senescence and systemic ageing

Author

Emad Manni, Nicola Jeffery, David Chambers, Luke Slade, Timothy Etheridge, and Lorna W. Harries

Subjects

miRNA, miR-361-5p, Human endothelial cells, Senescence, Lifespan, C. elegans, Medicine, Biology (General), QH301-705.5

Abstract

Senescent cells are key regulators of ageing and age-associated disease. MicroRNAs (miRs) are a key component of the molecular machinery governing cellular senescence, with several known to regulate important genes associated with this process.We sought to identify miRs associated with both senescence and reversal by pinpointing those showing opposing directionality of effect in senescence and in response to senotherapy. Cellular senescence phenotypes were assessed in primary human endothelial cells following targeted manipulation of emergent miRNAs. Finally, the effect of conserved target gene knockdown on lifespan and healthspan was assessed in a C. elegans system in vivo.Three miRNAs (miR-5787, miR-3665 and miR-361-5p) demonstrated associations with both senescence and rejuvenation, but miR-361-5p alone demonstrated opposing effects in senescence and rescue. Treatment of late passage human endothelial cells with a miR-361-5p mimic caused a 14 % decrease in the senescent load of the culture. RNAi gene knockdown of conserved miR-361-5p target genes in a C. elegans model however resulted in adverse effects on healthspan and/or lifespan.Although miR-361-5p may attenuate aspects of the senescence phenotype in human primary endothelial cells, many of its validated target genes also play essential roles in the regulation or formation of the cytoskeletal network, or its interaction with the extracellular matrix. These processes are essential for cell survival and cell function. Targeting miR-361-5p alone may not represent a promising target for future senotherapy; more sophisticated approaches to attenuate its interaction with specific targets without roles in essential cell processes would be required.

Published

2023

4. Changes to the identity of EndoC-βH1 beta cells may be mediated by stress-induced depletion of HNRNPD

Author

Nicola Jeffery, David Chambers, Brandon M. Invergo, Ryan M. Ames, and Lorna W. Harries

Subjects

Beta-cells, Cell differentiation, HNRNPD, RNA binding proteins, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Abstract Background Beta cell identity changes occur in the islets of donors with diabetes, but the molecular basis of this remains unclear. Protecting residual functional beta cells from cell identity changes may be beneficial for patients with diabetes. Results A somatostatin-positive cell population was induced in stressed clonal human EndoC-βH1 beta cells and was isolated using FACS. A transcriptomic characterisation of somatostatin-positive cells was then carried out. Gain of somatostatin-positivity was associated with marked dysregulation of the non-coding genome. Very few coding genes were differentially expressed. Potential candidate effector genes were assessed by targeted gene knockdown. Targeted knockdown of the HNRNPD gene induced the emergence of a somatostatin-positive cell population in clonal EndoC-βH1 beta cells comparable with that we have previously reported in stressed cells. Conclusions We report here a role for the HNRNPD gene in determination of beta cell identity in response to cellular stress. These findings widen our understanding of the role of RNA binding proteins and RNA biology in determining cell identity and may be important for protecting remaining beta cell reserve in diabetes.

Published

2021

5. Gene expression analysis reveals a 5-gene signature for progression-free survival in prostate cancer

Author

Zhuofan Mou, Jack Spencer, Bridget Knight, Joseph John, Paul McCullagh, John S. McGrath, and Lorna W. Harries

Subjects

gene signature, prostate cancer, transcriptomics, prognosis, prediction model, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Prostate cancer (PCa) is the second most common male cancer worldwide, but effective biomarkers for the presence or progression risk of disease are currently elusive. In a series of nine matched histologically confirmed PCa and benign samples, we carried out an integrated transcriptome-wide gene expression analysis, including differential gene expression analysis and weighted gene co-expression network analysis (WGCNA), which identified a set of potential gene markers highly associated with tumour status (malignant vs. benign). We then used these genes to establish a minimal progression-free survival (PFS)-associated gene signature (GS) (PCBP1, PABPN1, PTPRF, DANCR, and MYC) using least absolute shrinkage and selection operator (LASSO) and stepwise multivariate Cox regression analyses from The Cancer Genome Atlas prostate adenocarcinoma (TCGA-PRAD) dataset. Our signature was able to predict PFS over 1, 3, and 5 years in TCGA-PRAD dataset, with area under the curve (AUC) of 0.64–0.78, and our signature remained as a prognostic factor independent of age, Gleason score, and pathological T and N stages. A nomogram combining the signature and Gleason score demonstrated improved predictive capability for PFS (AUC: 0.71–0.85) and was superior to the Cambridge Prognostic Group (CPG) model alone and some conventionally used clinicopathological factors in predicting PFS. In conclusion, we have identified and validated a novel five-gene signature and established a nomogram that effectively predicted PFS in patients with PCa. Findings may improve current prognosis tools for PFS and contribute to clinical decision-making in PCa treatment.

Published

2022

6. Transcriptomic meta‐analysis of disuse muscle atrophy vs. resistance exercise‐induced hypertrophy in young and older humans

Author

Colleen S. Deane, Craig R.G. Willis, Bethan E. Phillips, Philip J. Atherton, Lorna W. Harries, Ryan M. Ames, Nathaniel J. Szewczyk, and Timothy Etheridge

Subjects

Skeletal muscle disuse, Resistance exercise training, Ageing, Transcriptomic meta‐analysis, Gene‐level analysis, Network analysis, Diseases of the musculoskeletal system, RC925-935, Human anatomy, QM1-695

Abstract

Abstract Background Skeletal muscle atrophy manifests across numerous diseases; however, the extent of similarities/differences in causal mechanisms between atrophying conditions in unclear. Ageing and disuse represent two of the most prevalent and costly atrophic conditions, with resistance exercise training (RET) being the most effective lifestyle countermeasure. We employed gene‐level and network‐level meta‐analyses to contrast transcriptomic signatures of disuse and RET, plus young and older RET to establish a consensus on the molecular features of, and therapeutic targets against, muscle atrophy in conditions of high socio‐economic relevance. Methods Integrated gene‐level and network‐level meta‐analysis was performed on publicly available microarray data sets generated from young (18–35 years) m. vastus lateralis muscle subjected to disuse (unilateral limb immobilization or bed rest) lasting ≥7 days or RET lasting ≥3 weeks, and resistance‐trained older (≥60 years) muscle. Results Disuse and RET displayed predominantly separate transcriptional responses, and transcripts altered across conditions were mostly unidirectional. However, disuse and RET induced directly inverted expression profiles for mitochondrial function and translation regulation genes, with COX4I1, ENDOG, GOT2, MRPL12, and NDUFV2, the central hub components of altered mitochondrial networks, and ZMYND11, a hub gene of altered translation regulation. A substantial number of genes (n = 140) up‐regulated post‐RET in younger muscle were not similarly up‐regulated in older muscle, with young muscle displaying a more pronounced extracellular matrix (ECM) and immune/inflammatory gene expression response. Both young and older muscle exhibited similar RET‐induced ubiquitination/RNA processing gene signatures with associated PWP1, PSMB1, and RAF1 hub genes. Conclusions Despite limited opposing gene profiles, transcriptional signatures of disuse are not simply the converse of RET. Thus, the mechanisms of unloading cannot be derived from studying muscle loading alone and provides a molecular basis for understanding why RET fails to target all transcriptional features of disuse. Loss of RET‐induced ECM mechanotransduction and inflammatory profiles might also contribute to suboptimal ageing muscle adaptations to RET. Disuse and age‐dependent molecular candidates further establish a framework for understanding and treating disuse/ageing atrophy.

Published

2021

7. Islet-expressed circular RNAs are associated with type 2 diabetes status in human primary islets and in peripheral blood

Author

Shahnaz Haque, Ryan M. Ames, Karen Moore, Benjamin P. Lee, Nicola Jeffery, and Lorna W. Harries

Subjects

circRNA, Diabetes, Human, islet, EndoC-βH1 beta cells, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Circular RNAs are non-coding RNA molecules with gene regulatory potential that have been associated with several human diseases. They are stable and present in the circulation, making them excellent candidates for biomarkers of disease. Despite their promise as biomarkers or future therapeutic targets, information on their expression and functionality in human pancreatic islets is a relatively unexplored subject. Methods Here we aimed to produce an enriched circRNAome profile for human pancreatic islets by CircleSeq, and to explore the relationship between circRNA expression, diabetes status, genotype at T2D risk loci and measures of glycaemia (insulin secretory index; SI and HbA1c) in human islet preparations from healthy control donors and donors with type 2 diabetes using ANOVA or linear regression as appropriate. We also assessed the effect of elevated glucose, cytokine and lipid and hypoxia on circRNA expression in the human beta cell line EndoC-βH1. Results We identified over 2600 circRNAs present in human islets. Of the five most abundant circRNAs in human islets, four (circCIRBP, circZKSCAN, circRPH3AL and circCAMSAP1) demonstrated marked associations with diabetes status. CircCIRBP demonstrated an association with insulin secretory index in isolated human islets and circCIRBP and circRPH3AL displayed altered expression with elevated fatty acid in treated EndoC-βH1 cells. CircCAMSAP1 was also noted to be associated with T2D status in human peripheral blood. No associations between circRNA expression and genotype at T2D risk loci were identified in our samples. Conclusions Our data suggest that circRNAs are abundantly expressed in human islets, and that some are differentially regulated in the islets of donors with type 2 diabetes. Some islet circRNAs are also expressed in peripheral blood and the expression of one, circCAMSAP1, correlates with diabetes status. These findings highlight the potential of circRNAs as biomarkers for T2D.

Published

2020

8. Obesity impacts the regulation of miR-10b and its targets in primary breast tumors

Author

Ari Meerson, Yaniv Eliraz, Hila Yehuda, Bridget Knight, Malcolm Crundwell, Douglas Ferguson, Benjamin P. Lee, and Lorna W. Harries

Subjects

miR-10b, Breast cancer, Obesity, microRNA, Tumor suppressors, Oncogenes, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Obesity increases breast cancer (BC) risk in post-menopausal women by mostly unknown molecular mechanisms which may partly be regulated by microRNAs (miRNAs). Methods We isolated RNA from paired benign and malignant biopsies from 83 BC patients and determined miRNA profiles in samples from 12 women at the extremes of the BMI distribution by RNA-seq. Candidates were validated in all samples. Associations between miR-10b expression and validated target transcript levels, and effects of targeted manipulation of miR-10b levels in a primary BC cell line on proliferation and invasion potential, were explored. Results Of the 148 miRNAs robustly expressed in breast tissues, the levels of miR-21, miR-10b, miR-451a, miR-30c, and miR-378d were significantly associated with presence of cancer. Of these, miR-10b showed a stronger down-regulation in the tumors of the obese subjects, as opposed to the lean. In ductal but not lobular tumors, significant inverse correlations were observed between the tumor levels of miR-10b and miR-30c and the mRNA levels of cancer-relevant target genes SRSF1, PIEZO1, MAPRE1, CDKN2A, TP-53 and TRA2B, as well as tumor grade. Suppression of miR-10b levels in BT-549 primary BC–derived cells increased cell proliferation and invasive capacity, while exogenous miR-10b mimic decreased invasion. Manipulation of miR-10b levels also inversely affected the mRNA levels of miR-10b targets BCL2L11, PIEZO1 and NCOR2. Conclusions Our findings suggest that miR-10b may be a mediator between obesity and cancer in post-menopausal women, regulating several known cancer-relevant genes. MiR-10b expression may have diagnostic and therapeutic implications for the incidence and prognosis of BC in obese women.

Published

2019

9. Small molecule modulation of splicing factor expression is associated with rescue from cellular senescence

Author

Eva Latorre, Vishal C. Birar, Angela N. Sheerin, J. Charles C. Jeynes, Amy Hooper, Helen R. Dawe, David Melzer, Lynne S. Cox, Richard G. A. Faragher, Elizabeth L. Ostler, and Lorna W. Harries

Subjects

Alternative splicing, Ageing, Resveratrol, Senescence, Fibroblasts, Cytology, QH573-671

Abstract

Abstract Background Altered expression of mRNA splicing factors occurs with ageing in vivo and is thought to be an ageing mechanism. The accumulation of senescent cells also occurs in vivo with advancing age and causes much degenerative age-related pathology. However, the relationship between these two processes is opaque. Accordingly we developed a novel panel of small molecules based on resveratrol, previously suggested to alter mRNA splicing, to determine whether altered splicing factor expression had potential to influence features of replicative senescence. Results Treatment with resveralogues was associated with altered splicing factor expression and rescue of multiple features of senescence. This rescue was independent of cell cycle traverse and also independent of SIRT1, SASP modulation or senolysis. Under growth permissive conditions, cells demonstrating restored splicing factor expression also demonstrated increased telomere length, re-entered cell cycle and resumed proliferation. These phenomena were also influenced by ERK antagonists and agonists. Conclusions This is the first demonstration that moderation of splicing factor levels is associated with reversal of cellular senescence in human primary fibroblasts. Small molecule modulators of such targets may therefore represent promising novel anti-degenerative therapies.

Published

2017

10. The cancer-associated cell migration protein TSPAN1 is under control of androgens and its upregulation increases prostate cancer cell migration

Author

Jennifer Munkley, Urszula L. McClurg, Karen E. Livermore, Ingrid Ehrmann, Bridget Knight, Paul Mccullagh, John Mcgrath, Malcolm Crundwell, Lorna W. Harries, Hing Y. Leung, Ian G. Mills, Craig N. Robson, Prabhakar Rajan, and David J. Elliott

Subjects

Medicine, Science

Abstract

Abstract Cell migration drives cell invasion and metastatic progression in prostate cancer and is a major cause of mortality and morbidity. However the mechanisms driving cell migration in prostate cancer patients are not fully understood. We previously identified the cancer-associated cell migration protein Tetraspanin 1 (TSPAN1) as a clinically relevant androgen regulated target in prostate cancer. Here we find that TSPAN1 is acutely induced by androgens, and is significantly upregulated in prostate cancer relative to both normal prostate tissue and benign prostate hyperplasia (BPH). We also show for the first time, that TSPAN1 expression in prostate cancer cells controls the expression of key proteins involved in cell migration. Stable upregulation of TSPAN1 in both DU145 and PC3 cells significantly increased cell migration and induced the expression of the mesenchymal markers SLUG and ARF6. Our data suggest TSPAN1 is an androgen-driven contributor to cell survival and motility in prostate cancer.

Published

2017

11. RNA Biology Provides New Therapeutic Targets for Human Disease

Author

Lorna W. Harries

Subjects

mRNA processing, RNA editing, RNA export, RNA therapeutics, ncRNA, splicing, Genetics, QH426-470

Abstract

RNA is the messenger molecule that conveys information from the genome and allows the production of biomolecules required for life in a responsive and regulated way. Most genes are able to produce multiple mRNA products in response to different internal or external environmental signals, in different tissues and organs, and at specific times in development or later life. This fine tuning of gene expression is dependent on the coordinated effects of a large and intricate set of regulatory machinery, which together orchestrate the genomic output at each locus and ensure that each gene is expressed at the right amount, at the right time and in the correct location. This complexity of control, and the requirement for both sequence elements and the entities that bind them, results in multiple points at which errors may occur. Errors of RNA biology are common and found in association with both rare, single gene disorders, but also more common, chronic diseases. Fortunately, complexity also brings opportunity. The existence of many regulatory steps also offers multiple levels of potential therapeutic intervention which can be exploited. In this review, I will outline the specific points at which coding RNAs may be regulated, indicate potential means of intervention at each stage, and outline with examples some of the progress that has been made in this area. Finally, I will outline some of the remaining challenges with the delivery of RNA-based therapeutics but indicate why there are reasons for optimism.

Published

2019

12. Glycosylation is an Androgen-Regulated Process Essential for Prostate Cancer Cell Viability

Author

Jennifer Munkley, Daniel Vodak, Karen E. Livermore, Katherine James, Brian T. Wilson, Bridget Knight, Paul Mccullagh, John Mcgrath, Malcolm Crundwell, Lorna W. Harries, Hing Y. Leung, Craig N. Robson, Ian G. Mills, Prabhakar Rajan, and David J. Elliott

Subjects

Medicine, Medicine (General), R5-920

Abstract

Steroid androgen hormones play a key role in the progression and treatment of prostate cancer, with androgen deprivation therapy being the first-line treatment used to control cancer growth. Here we apply a novel search strategy to identify androgen-regulated cellular pathways that may be clinically important in prostate cancer. Using RNASeq data, we searched for genes that showed reciprocal changes in expression in response to acute androgen stimulation in culture, and androgen deprivation in patients with prostate cancer. Amongst 700 genes displaying reciprocal expression patterns we observed a significant enrichment in the cellular process glycosylation. Of 31 reciprocally-regulated glycosylation enzymes, a set of 8 (GALNT7, ST6GalNAc1, GCNT1, UAP1, PGM3, CSGALNACT1, ST6GAL1 and EDEM3) were significantly up-regulated in clinical prostate carcinoma. Androgen exposure stimulated synthesis of glycan structures downstream of this core set of regulated enzymes including sialyl-Tn (sTn), sialyl LewisX (SLeX), O-GlcNAc and chondroitin sulphate, suggesting androgen regulation of the core set of enzymes controls key steps in glycan synthesis. Expression of each of these enzymes also contributed to prostate cancer cell viability. This study identifies glycosylation as a global target for androgen control, and suggests loss of specific glycosylation enzymes might contribute to tumour regression following androgen depletion therapy.

Published

2016

13. Androgen-regulated transcription of ESRP2 drives alternative splicing patterns in prostate cancer

Author

Jennifer Munkley, Ling Li, S R Gokul Krishnan, Gerald Hysenaj, Emma Scott, Caroline Dalgliesh, Htoo Zarni Oo, Teresa Mendes Maia, Kathleen Cheung, Ingrid Ehrmann, Karen E Livermore, Hanna Zielinska, Oliver Thompson, Bridget Knight, Paul McCullagh, John McGrath, Malcolm Crundwell, Lorna W Harries, Mads Daugaard, Simon Cockell, Nuno L Barbosa-Morais, Sebastian Oltean, and David J Elliott

Subjects

RNA, splicing, gene expression, cancer, Medicine, Science, Biology (General), QH301-705.5

Abstract

Prostate is the most frequent cancer in men. Prostate cancer progression is driven by androgen steroid hormones, and delayed by androgen deprivation therapy (ADT). Androgens control transcription by stimulating androgen receptor (AR) activity, yet also control pre-mRNA splicing through less clear mechanisms. Here we find androgens regulate splicing through AR-mediated transcriptional control of the epithelial-specific splicing regulator ESRP2. Both ESRP2 and its close paralog ESRP1 are highly expressed in primary prostate cancer. Androgen stimulation induces splicing switches in many endogenous ESRP2-controlled mRNA isoforms, including splicing switches correlating with disease progression. ESRP2 expression in clinical prostate cancer is repressed by ADT, which may thus inadvertently dampen epithelial splice programmes. Supporting this, treatment with the AR antagonist bicalutamide (Casodex) induced mesenchymal splicing patterns of genes including FLNB and CTNND1. Our data reveals a new mechanism of splicing control in prostate cancer with important implications for disease progression.

Published

2019

14. Dysregulated RNA processing and metabolism: a new hallmark of ageing and provocation for cellular senescence

Author

Lorna W. Harries

Subjects

Cell Biology, Molecular Biology, Biochemistry

Abstract

The human genome is capable of producing hundreds of thousands of different proteins and non-coding RNAs from20 000 genes, in a co-ordinated and regulated fashion. This is achieved by a collection of phenomena known as mRNA processing and metabolism, and encompasses events in the life cycle of an RNA from synthesis to degradation. These factors are critical determinants of cellular adaptability and plasticity, which allows the cell to adjust its transcriptomic output in response to its internal and external environment. Evidence is building that dysfunctional RNA processing and metabolism may be a key contributor to the development of cellular senescence. Senescent cells by definition have exited cell cycle, but have gained functional features such as the secretion of the senescence-associated secretory phenotype (SASP), a known driver of chronic disease and perhaps even ageing itself. In this review, I will outline the impact of dysregulated mRNA processing and metabolism on senescence and ageing at the level of genes, cells and systems, and describe the mechanisms by which progressive deterioration in these processes may impact senescence and organismal ageing. Finally, I will present the evidence implicating this important process as a new hallmark of ageing, which could be harnessed in the future to develop new senotherapeutic interventions for chronic disease.

Published

2022

15. Persistence of clinically relevant levels of SARS-CoV2 envelope gene subgenomic RNAs in non-immunocompromised individuals

Author

Merlin Davies, Laura R Bramwell, Nicola Jeffery, Ben Bunce, Ben P Lee, Bridget Knight, Cressida Auckland, Jane AH Masoli, and Lorna W Harries

Subjects

Microbiology (medical), SARS-CoV-2, transmission, COVID-19, sgRNA, subgenomic RNA, persistence, General Medicine, Viral Load, Article, Infectious Diseases, Humans, RNA, Viral, sgRNA, Retrospective Studies

Abstract

Objectives This study aimed to evaluate the associations between COVID-19 severity and active viral load, and to characterize the dynamics of active SARS-CoV-2 clearance in a series of archival samples taken from patients in the first wave of COVID-19 infection in the South West of the UK. Methods Subgenomic RNA (sgRNA) and E-gene genomic sequences were measured in a retrospective collection of PCR-confirmed SARS-CoV-2-positive samples from 176 individuals, and related to disease severity. Viral clearance dynamics were then assessed in relation to symptom onset and last positive test. Results Whilst E-gene sgRNAs declined before E-gene genomic sequences, some individuals retained sgRNA positivity for up to 68 days. 13% of sgRNA-positive cases still exhibited clinically relevant levels of virus after 10 days, with no clinical features previously associated with prolonged viral clearance times. Conclusions Our results suggest that potentially active virus can sometimes persist beyond a 10-day period, and could pose a potential risk of onward transmission. Where this would pose a serious public health threat, additional mitigation strategies may be necessary to reduce the risk of secondary cases in vulnerable settings.

Published

2022

16. Senotherapeutic Drugs: A New Avenue for Skincare?

Author

Ben P. Lee and Lorna W. Harries

Subjects

business.industry, Cellular senescence, Context (language use), Skin Care, Skin Aging, Senotherapeutics, Humans, Rejuvenation, Medicine, Health maintenance, Surgery, business, Neuroscience, Cellular Senescence

Abstract

SUMMARY Skin aging is an outward manifestation of other cellular and molecular aging processes occurring elsewhere in the body. These processes are known collectively as the "hallmarks" of aging, which are a series of basic health maintenance mechanisms that fail over time. Cellular senescence is one of the most studied of the hallmarks of aging; senescent cells accumulate over time and are major drives of the aging process. Here, we discuss the impact of cellular senescence in the context of skin aging, and discuss the emerging landscape of interventions designed for their selective removal by targeted cell death (senolytics) or rejuvenation (senomorphics). We discuss the serotherapeutic strategies that are currently under investigation for systemic aging, which may bring eventual benefits for skin health. Next, we discuss a newly discovered hallmark of aging, dysregulated mRNA processing, which can be targeted for the senomorphic effect. Finally, we highlight a new modality for manipulation of disrupted mRNA processing, oligonucleotide therapeutics. The emerging field of senotherapeutics is set to revolutionize how we view and treat skin aging, and senotherapies are now poised to become a new class of skincare interventions.

Published

2021

17. Vaccine escape, increased breakthrough and reinfection in infliximab-treated patients with IBD during the Omicron wave of the SARS-CoV-2 pandemic

Author

Nicholas A Kennedy, Malik Janjua, Neil Chanchlani, Simeng Lin, Claire Bewshea, Rachel Nice, Timothy J McDonald, Cressida Auckland, Lorna W Harries, Merlin Davies, Stephen Michell, Klaartje B Kok, Christopher A Lamb, Philip J Smith, Ailsa L Hart, Richard CG Pollok, Charlie W Lees, Rosemary J Boyton, Daniel M Altmann, Shaji Sebastian, Nicholas Powell, James R Goodhand, and Tariq Ahmad

Subjects

Vaccines, COVID-19 Vaccines, SARS-CoV-2, Reinfection, ChAdOx1 nCoV-19, Gastroenterology, Humans, COVID-19, Antibodies, Viral, Inflammatory Bowel Diseases, Pandemics, Infliximab, BNT162 Vaccine

Abstract

ObjectiveAntitumour necrosis factor (TNF) drugs impair serological responses following SARS-CoV-2 vaccination. We sought to assess if a third dose of a messenger RNA (mRNA)-based vaccine substantially boosted anti-SARS-CoV-2 antibody responses and protective immunity in infliximab-treated patients with IBD.DesignThird dose vaccine induced anti-SARS-CoV-2 spike (anti-S) receptor-binding domain (RBD) antibody responses, breakthrough SARS-CoV-2 infection, reinfection and persistent oropharyngeal carriage in patients with IBD treated with infliximab were compared with a reference cohort treated with vedolizumab from the impaCt of bioLogic therApy on saRs-cov-2 Infection and immuniTY (CLARITY) IBD study.ResultsGeometric mean (SD) anti-S RBD antibody concentrations increased in both groups following a third dose of an mRNA-based vaccine. However, concentrations were lower in patients treated with infliximab than vedolizumab, irrespective of whether their first two primary vaccine doses were ChAdOx1 nCoV-19 (1856 U/mL (5.2) vs 10 728 U/mL (3.1), pCompared with vedolizumab-treated, infliximab-treated patients were more likely to experience SARS-CoV-2 breakthrough infection (HR 2.23 (95% CI 1.46 to 3.38), p=0.00018) and reinfection (HR 2.10 (95% CI 1.31 to 3.35), p=0.0019), but this effect was uncoupled from third vaccine dose anti-S RBD antibody concentrations. Reinfection occurred predominantly during the Omicron wave and was predicted by SARS-CoV-2 antinucleocapsid concentrations after the initial infection. We did not observe persistent oropharyngeal carriage of SARS-CoV-2. Hospitalisations and deaths were uncommon in both groups.ConclusionsFollowing a third dose of an mRNA-based vaccine, infliximab was associated with attenuated serological responses and more SARS-CoV-2 breakthrough infection and reinfection which were not predicted by the magnitude of anti-S RBD responses, indicative of vaccine escape by the Omicron variant.Trial registration numberISRCTN45176516.

Published

2022

18. Transcriptomic meta‐analysis of disuse muscle atrophy vs. resistance exercise‐induced hypertrophy in young and older humans

Author

Timothy Etheridge, Nathaniel J. Szewczyk, Lorna W. Harries, Colleen S. Deane, Bethan E. Phillips, Craig R. G. Willis, Ryan M. Ames, and Philip J. Atherton

Subjects

0301 basic medicine, medicine.medical_specialty, Vastus lateralis muscle, Skeletal muscle disuse, ENDOG, Diseases of the musculoskeletal system, Mechanotransduction, Cellular, Muscle hypertrophy, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Atrophy, Physiology (medical), Internal medicine, medicine, Humans, Orthopedics and Sports Medicine, Gene‐level analysis, Muscle, Skeletal, Aged, Resistance exercise training, Microarray analysis techniques, business.industry, QM1-695, Resistance Training, Original Articles, Hypertrophy, medicine.disease, Muscle atrophy, Ageing, Muscular Atrophy, COX4I1, 030104 developmental biology, Endocrinology, RC925-935, Transcriptomic meta‐analysis, 030220 oncology & carcinogenesis, Human anatomy, Original Article, Network analysis, medicine.symptom, business

Abstract

Background Skeletal muscle atrophy manifests across numerous diseases; however, the extent of similarities/differences in causal mechanisms between atrophying conditions in unclear. Ageing and disuse represent two of the most prevalent and costly atrophic conditions, with resistance exercise training (RET) being the most effective lifestyle countermeasure. We employed gene‐level and network‐level meta‐analyses to contrast transcriptomic signatures of disuse and RET, plus young and older RET to establish a consensus on the molecular features of, and therapeutic targets against, muscle atrophy in conditions of high socio‐economic relevance. Methods Integrated gene‐level and network‐level meta‐analysis was performed on publicly available microarray data sets generated from young (18–35 years) m. vastus lateralis muscle subjected to disuse (unilateral limb immobilization or bed rest) lasting ≥7 days or RET lasting ≥3 weeks, and resistance‐trained older (≥60 years) muscle. Results Disuse and RET displayed predominantly separate transcriptional responses, and transcripts altered across conditions were mostly unidirectional. However, disuse and RET induced directly inverted expression profiles for mitochondrial function and translation regulation genes, with COX4I1, ENDOG, GOT2, MRPL12, and NDUFV2, the central hub components of altered mitochondrial networks, and ZMYND11, a hub gene of altered translation regulation. A substantial number of genes (n = 140) up‐regulated post‐RET in younger muscle were not similarly up‐regulated in older muscle, with young muscle displaying a more pronounced extracellular matrix (ECM) and immune/inflammatory gene expression response. Both young and older muscle exhibited similar RET‐induced ubiquitination/RNA processing gene signatures with associated PWP1, PSMB1, and RAF1 hub genes. Conclusions Despite limited opposing gene profiles, transcriptional signatures of disuse are not simply the converse of RET. Thus, the mechanisms of unloading cannot be derived from studying muscle loading alone and provides a molecular basis for understanding why RET fails to target all transcriptional features of disuse. Loss of RET‐induced ECM mechanotransduction and inflammatory profiles might also contribute to suboptimal ageing muscle adaptations to RET. Disuse and age‐dependent molecular candidates further establish a framework for understanding and treating disuse/ageing atrophy.

Published

2021

19. Negligible senescence in naked mole rats may be a consequence of well-maintained splicing regulation

Author

Benjamin P. Lee, R. Buffenstein, M. Smith, and Lorna W. Harries

Subjects

0301 basic medicine, Senescence, Aging, Heterocephalus glaber, Longevity, DNA repair, Biology, Naked mole-rat, Srsfs, Klotho, Splicing factors, Mice, CDKN2A, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, Animals, Negligible senescence, Gene, Mole Rats, Alternative splicing, Brain, biology.organism_classification, hnRNPs, Phenotype, Cell biology, Ageing, 030104 developmental biology, RNA splicing, Original Article, RNA Splicing Factors, Cognitive function, Geriatrics and Gerontology, 030217 neurology & neurosurgery

Abstract

Naked mole-rats (NMRs) have amongst the longest lifespans relative to body size of any known, non-volant mammalian species. They also display an enhanced stress resistance phenotype, negligible senescence and very rarely are they burdened with chronic age-related diseases. Alternative splicing (AS) dysregulation is emerging as a potential driver of senescence and ageing. We hypothesised that the expression of splicing factors, important regulators of patterns of AS, may differ in NMRs when compared to other species with relatively shorter lifespans. We designed assays specific to NMR splicing regulatory factors and also to a panel of pre-selected brain-expressed genes known to demonstrate senescence-related alterations in AS in other species, and measured age-related changes in the transcript expression levels of these using embryonic and neonatal developmental stages through to extreme old age in NMR brain samples. We also compared splicing factor expression in both young mouse and NMR spleen and brain samples. Both NMR tissues showed approximately double the expression levels observed in tissues from similarly sized mice. Furthermore, contrary to observations in other species, following a brief period of labile expression in early life stages, adult NMR splicing factors and patterns of AS for functionally relevant brain genes remained remarkably stable for at least two decades. These findings are consistent with a model whereby the conservation of splicing regulation and stable patterns of AS may contribute to better molecular stress responses and the avoidance of senescence in NMRs, contributing to their exceptional lifespan and prolonged healthspan. Electronic supplementary material The online version of this article (10.1007/s11357-019-00150-7) contains supplementary material, which is available to authorized users.

Published

2020

20. A biallelic SNIP1 Amish founder variant causes a recognizable neurodevelopmental disorder

Author

Hannah Jones, Tom Herr, Lorna W. Harries, Erik G. Puffenberger, Rebecca Evans, Harold E. Cross, Olivia Wenger, Angela Scheid, Ethan M. Scott, Jim Deline, Joanna Kennedy, Emma L. Baple, Lettie E. Rawlins, Zineb Ammous, Ryan M. Ames, Joseph S Leslie, Andrew H. Crosby, and Barry A. Chioza

Subjects

Cell signaling, Cancer Research, Heredity, Gene Expression, Signal transduction, QH426-470, Biochemistry, Homozygosity, Medical Conditions, Neurodevelopmental disorder, Intellectual disability, Gene expression, Medicine and Health Sciences, Global developmental delay, Musculoskeletal System, Genetics (clinical), Genetics, Transcriptional Control, RNA-Binding Proteins, SMAD NUCLEAR INTERACTING PROTEIN 1, Hypotonia, Phenotypes, Neurology, Anatomy, medicine.symptom, Research Article, Cell biology, Spliceosome, SMAD signaling, Genes, Recessive, Biology, Developmental Neuroscience, DNA-binding proteins, medicine, Humans, Gene Regulation, Craniofacial, Molecular Biology, Skeleton, Alleles, Ecology, Evolution, Behavior and Systematics, Skull, Biology and Life Sciences, Proteins, medicine.disease, Regulatory Proteins, Neurodevelopmental Disorders, Amish, Neuroscience, Transcription Factors

Abstract

SNIP1 (Smad nuclear interacting protein 1) is a widely expressed transcriptional suppressor of the TGF-β signal-transduction pathway which plays a key role in human spliceosome function. Here, we describe extensive genetic studies and clinical findings of a complex inherited neurodevelopmental disorder in 35 individuals associated with a SNIP1 NM_024700.4:c.1097A>G, p.(Glu366Gly) variant, present at high frequency in the Amish community. The cardinal clinical features of the condition include hypotonia, global developmental delay, intellectual disability, seizures, and a characteristic craniofacial appearance. Our gene transcript studies in affected individuals define altered gene expression profiles of a number of molecules with well-defined neurodevelopmental and neuropathological roles, potentially explaining clinical outcomes. Together these data confirm this SNIP1 gene variant as a cause of an autosomal recessive complex neurodevelopmental disorder and provide important insight into the molecular roles of SNIP1, which likely explain the cardinal clinical outcomes in affected individuals, defining potential therapeutic avenues for future research., Author summary Neurodevelopmental disorders are a group of conditions that may be inherited in families, characterized by impairments of the growth, development and function of the brain. This may result in neuropsychiatric problems, impaired motor function, impaired learning, language and/or non-verbal communication. These conditions may be associated with epilepsy, characterised by recurrent abnormal electrical activity in the brain. Here we confirm a founder SNIP1 gene variant as a cause of an autosomal recessive complex neurodevelopmental disorder in the Amish. We provide a detailed description of the clinical features of the condition alongside clinical management recommendations. Our genetic studies identify altered gene expression patterns in affected children associated with the SNIP1 genetic alteration. This identified abnormalities in several proteins with important roles in brain development and function, potentially explaining the clinical features of the condition.

Published

2021

21. Changes to the identity of EndoC-βH1 beta cells may be mediated by stress-induced depletion of HNRNPD

Author

Lorna W. Harries, Nicola Jeffery, Ryan M. Ames, Brandon M. Invergo, and David J. Chambers

Subjects

0301 basic medicine, Beta-cells, QH301-705.5, Cellular differentiation, Cell, Population, QD415-436, Biology, Biochemistry, General Biochemistry, Genetics and Molecular Biology, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, HNRNPD Gene, Cell differentiation, medicine, HNRNPD, Biology (General), education, education.field_of_study, Gene knockdown, Research, Cell biology, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, RNA binding proteins, Beta cell, Stem cell, TP248.13-248.65, Biotechnology

Abstract

Background Beta cell identity changes occur in the islets of donors with diabetes, but the molecular basis of this remains unclear. Protecting residual functional beta cells from cell identity changes may be beneficial for patients with diabetes. Results A somatostatin-positive cell population was induced in stressed clonal human EndoC-βH1 beta cells and was isolated using FACS. A transcriptomic characterisation of somatostatin-positive cells was then carried out. Gain of somatostatin-positivity was associated with marked dysregulation of the non-coding genome. Very few coding genes were differentially expressed. Potential candidate effector genes were assessed by targeted gene knockdown. Targeted knockdown of the HNRNPD gene induced the emergence of a somatostatin-positive cell population in clonal EndoC-βH1 beta cells comparable with that we have previously reported in stressed cells. Conclusions We report here a role for the HNRNPD gene in determination of beta cell identity in response to cellular stress. These findings widen our understanding of the role of RNA binding proteins and RNA biology in determining cell identity and may be important for protecting remaining beta cell reserve in diabetes.

Published

2021

22. circRNAs expressed in human peripheral blood are associated with human aging phenotypes, cellular senescence and mouse lifespan

Author

Lorna W. Harries, Luanne L. Peters, Luigi Ferrucci, Shahnaz Haque, Stefania Bandinelli, Karen Moore, Luke C. Pilling, and Ryan M. Ames

Subjects

Median strain lifespan, 0301 basic medicine, Senescence, Aging, media_common.quotation_subject, Longevity, Disease, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Circular RNA, Gene expression, Animals, Humans, Cellular Senescence, Aged, media_common, Hand Strength, RNA, RNA, Circular, Aging phenotypes, Molecular medicine, Phenotype, Cell biology, MicroRNAs, 030104 developmental biology, Original Article, Geriatrics and Gerontology, 030217 neurology & neurosurgery

Abstract

Circular RNAs (circRNAs) are an emerging class of non-coding RNA molecules that are thought to regulate gene expression and human disease. Despite the observation that circRNAs are known to accumulate in older organisms and have been reported in cellular senescence, their role in aging remains relatively unexplored. Here, we have assessed circRNA expression in aging human blood and followed up age-associated circRNA in relation to human aging phenotypes, mammalian longevity as measured by mouse median strain lifespan and cellular senescence in four different primary human cell types. We found that circRNAs circDEF6, circEP300, circFOXO3 and circFNDC3B demonstrate associations with parental longevity or hand grip strength in 306 subjects from the InCHIANTI study of aging, and furthermore, circFOXO3 and circEP300 also demonstrate differential expression in one or more human senescent cell types. Finally, four circRNAs tested showed evidence of conservation in mouse. Expression levels of one of these, circPlekhm1, was nominally associated with lifespan. These data suggest that circRNA may represent a novel class of regulatory RNA involved in the determination of aging phenotypes, which may show future promise as both biomarkers and future therapeutic targets for age-related disease.

Published

2019

23. Astrocyte senescence may drive alterations in GFAPα, CDKN2A p14ARF, and TAU3 transcript expression and contribute to cognitive decline

Author

Nicholas J. Gutowski, Eva Latorre, Janet E. Holley, Jed J. Lye, Ben P. Lee, Lorna W. Harries, Stefania Bandinelli, and Luigi Ferrucci

Subjects

0301 basic medicine, Senescence, Aging, Alternative splicing, Biology, Phenotype, Cell biology, 03 medical and health sciences, Splicing factor, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, RNA splicing, Gene expression, medicine, Geriatrics and Gerontology, Cognitive decline, 030217 neurology & neurosurgery, Astrocyte

Abstract

The accumulation of senescent cells in tissues is causally linked to the development of several age-related diseases; the removal of senescent glial cells in animal models prevents Tau accumulation and cognitive decline. Senescent cells can arise through several distinct mechanisms; one such mechanism is dysregulation of alternative splicing. In this study, we characterised the senescent cell phenotype in primary human astrocytes in terms of SA-β-Gal staining and SASP secretion, and then assessed splicing factor expression and candidate gene splicing patterns. Finally, we assessed associations between expression of dysregulated isoforms and premature cognitive decline in 197 samples from the InCHIANTI study of ageing, where expression was present in both blood and brain. We demonstrate here that senescent astrocytes secrete a modified SASP characterised by increased IL8, MMP3, MMP10, and TIMP2 but decreased IL10 levels. We identified significant changes in splicing factor expression for 10/20 splicing factors tested in senescent astrocytes compared with early passage cells, as well as dysregulation of isoform levels for 8/13 brain or senescence genes tested. Finally, associations were identified between peripheral blood GFAPα, TAU3, and CDKN2A (P14ARF) isoform levels and mild or severe cognitive decline over a 3–7-year period. Our data are suggestive that some of the features of cognitive decline may arise from dysregulated splicing of important genes in senescent brain support cells, and that defects in alternative splicing or splicing regulator expression deserve exploration as points of therapeutic intervention in the future.

Published

2019

24. The Longevity-Associated SH2B3 (LNK) Genetic Variant: Selected Aging Phenotypes in 379,758 Subjects

Author

Luke C. Pilling, Luigi Ferrucci, Lorna W. Harries, David Melzer, Chia-Ling Kuo, Micaella Joaquim, and George A. Kuchel

Subjects

Oncology, Aging, medicine.medical_specialty, Geroscience, business.industry, media_common.quotation_subject, Longevity, Locus (genetics), Disease, Odds ratio, Confidence interval, Internal medicine, medicine, Geriatrics and Gerontology, Allele, Centenarian, business, media_common

Abstract

Human SH2B3 is involved in growth factor and inflammation signaling. A SH2B3 missense variant (rs3184504) is associated with cardiovascular diseases plus breast, colorectal, and lung cancers, with highly correlated variants across the ATXN2/SH2B3/BRAP locus linked to parental age at death, suggesting a geroscience common mechanism of aging and disease. To better understand the SH2B3-related aging pathway and its potential as an intervention target, we undertook a phenotype-wide association study (PheWAS) of 52 aging traits. Data were obtained from 379,758 European-descent UK Biobank participants, aged 40–70 at baseline: 27% of participants were CC homozygotes and 23% TT at rs3184504. Parental extreme longevity (mothers aged ≥98 years, fathers aged ≥96 years) was more common in CC versus TT (odds ratio [OR] = 1.18, 95% confidence interval [CI]: 1.07 to 1.29) with an additive per allele effect. The C allele associated with better cognitive function and white blood cell counts were more likely to be normal. The C allele reduced risks of coronary heart disease (OR = 0.95, 95% CI: 0.93 to 0.96) but was also associated with a modestly higher cancer rate (OR = 1.03, 95% CI: 1.02 to 1.04), suggesting a trade-off across aging outcomes and limiting its potential as an anti-aging target.

Published

2019

25. Cellular stressors may alter islet hormone cell proportions by moderation of alternative splicing patterns

Author

Noel G. Morgan, David J. Chambers, Sarah J. Richardson, Nicola Jeffery, and Lorna W. Harries

Subjects

endocrine system, Gene Expression, 030209 endocrinology & metabolism, Biology, Heterogeneous ribonucleoprotein particle, Cell Line, Islets of Langerhans, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, Neuroendocrine Cells, Stress, Physiological, Insulin-Secreting Cells, Gene expression, Genetics, Humans, Insulin, Protein Kinase Inhibitors, Molecular Biology, Gene, Genetics (clinical), 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Gene Expression Profiling, Alternative splicing, General Medicine, Endoplasmic Reticulum Stress, Glucagon, Cell biology, Gene expression profiling, Alternative Splicing, Glucose, Diabetes Mellitus, Type 2, RNA splicing, Cytokines, General Article

Abstract

Changes to islet cell identity in response to type 2 diabetes (T2D) have been reported in rodent models, but are less well characterized in humans. We assessed the effects of aspects of the diabetic microenvironment on hormone staining, total gene expression, splicing regulation and the alternative splicing patterns of key genes in EndoC-βH1 human beta cells. Genes encoding islet hormones [somatostatin (SST), insulin (INS), Glucagon (GCG)], differentiation markers [Forkhead box O1 (FOXO1), Paired box 6, SRY box 9, NK6 Homeobox 1, NK6 Homeobox 2] and cell stress markers (DNA damage inducible transcript 3, FOXO1) were dysregulated in stressed EndoC-βH1 cells, as were some serine arginine rich splicing factor splicing activator and heterogeneous ribonucleoprotein particle inhibitor genes. Whole transcriptome analysis of primary T2D islets and matched controls demonstrated dysregulated splicing for ~25% of splicing events, of which genes themselves involved in messenger ribonucleic acid processing and regulation of gene expression comprised the largest group. Approximately 5% of EndoC-βH1 cells exposed to these factors gained SST positivity in vitro. An increased area of SST staining was also observed ex vivo in pancreas sections recovered at autopsy from donors with type 1 diabetes (T1D) or T2D (9.3% for T1D and 3% for T2D, respectively compared with 1% in controls). Removal of the stressful stimulus or treatment with the AKT Serine/Threonine kinase inhibitor SH-6 restored splicing factor expression and reversed both hormone staining effects and patterns of gene expression. This suggests that reversible changes in hormone expression may occur during exposure to diabetomimetic cellular stressors, which may be mediated by changes in splicing regulation.

Published

2019

26. Extreme longevity variants at the FOXO3 locus may moderate FOXO3 isoform levels

Author

Richard C. Allsopp, Francis B. Stephens, D. Craig Willcox, Timothy A. Donlon, Bradley J. Willcox, Lorna W. Harries, Bridget A. Knight, Trevor Torigoe, Ryan Frankum, Tom S O Jameson, and Benjamin T. Wall

Subjects

Gene isoform, Genetics, Aging, media_common.quotation_subject, Forkhead Box Protein O3, Longevity, Skeletal muscle, Single-nucleotide polymorphism, Locus (genetics), Biology, Polymorphism, Single Nucleotide, medicine.anatomical_structure, Regulatory sequence, medicine, FOXO3, Humans, Protein Isoforms, Geriatrics and Gerontology, Allele, Alleles, media_common

Abstract

The rs2802292, rs2764264 and rs13217795 variants of FOXO3 have been associated with extreme longevity in multiple human populations, but the mechanisms underpinning this remain unclear. We aimed to characterise potential effects of longevity-associated variation on the expression and mRNA processing of the FOXO3 gene. We performed a comprehensive assessment of FOXO3 isoform usage across a wide variety of human tissues and carried out a bioinformatic analysis of the potential for longevity-associated variants to disrupt regulatory regions involved in isoform choice. We then related the expression of full length and 5′ truncated FOXO3 isoforms to rs13217795 genotype in peripheral blood and skeletal muscle from individuals of different rs13217795 genotypes. FOXO3 isoforms displayed considerable tissue specificity. We determined that rs13231195 and its tightly aligned proxy variant rs9400239 may lie in regulatory regions involved in isoform choice. The longevity allele at rs13217795 was associated with increased levels of full length FOXO3 isoforms in peripheral blood and a decrease in truncated FOXO3 isoforms in skeletal muscle RNA. We suggest that the longevity effect of FOXO3 SNPs may in part derive from a shift in isoform usage in skeletal muscle away from the production of 5′ truncated FOXO3 isoforms lacking a complete forkhead DNA binding domain, which may have compromised functionality.

Published

2021

27. Targeting Alternative Splicing for Reversal of Cellular Senescence in the Context of Aesthetic Aging

Author

Lorna W. Harries and Laura R. Bramwell

Subjects

Senescence, Aging, Cell cycle checkpoint, Esthetics, Dasatinib, Drug Evaluation, Preclinical, Oligonucleotides, Cellular senescence, Context (language use), 030230 surgery, Antioxidants, Skin Aging, 03 medical and health sciences, 0302 clinical medicine, Medicine, Animals, Humans, Protein Kinase Inhibitors, Cellular Senescence, Skin, Clinical Trials as Topic, Serine-Arginine Splicing Factors, business.industry, Alternative splicing, Extracellular Matrix, Alternative Splicing, 030220 oncology & carcinogenesis, RNA splicing, Models, Animal, Molecular mechanism, Surgery, Quercetin, business, Neuroscience

Abstract

SUMMARY Cellular senescence is a state of stable cell cycle arrest that has increasingly been linked with cellular, tissue, and organismal aging; targeted removal of senescent cells brings healthspan and lifespan benefits in animal models. Newly emerging approaches to specifically ablate or rejuvenate senescent cells are now the subject of intense study to explore their utility to provide novel treatments for the aesthetic signs and diseases of aging in humans. Here, we discuss different strategies that are being trialed in vitro, and more recently in vivo, for the targeted removal or reversal of senescent cells. Finally, we describe the evidence for a newly emerging molecular mechanism that may underpin senescence; dysregulation of alternative splicing. We will explore the potential of restoring splicing regulation as a novel "senotherapeutic" approach and discuss strategies by which this could be integrated into the established portfolio of skin aging therapeutics.

Published

2020

28. Small molecule modulation of splicing factor expression is associated with rescue from cellular senescence

Author

J. Charles C. Jeynes, David Melzer, Amy Hooper, Helen R. Dawe, Eva Latorre, Lynne S. Cox, Vishal C. Birar, Richard G. A. Faragher, Elizabeth L. Ostler, Angela Sheerin, and Lorna W. Harries

Subjects

0301 basic medicine, RNA Splicing Factors, Senescence, MAPK/ERK pathway, Biology, Small Molecule Libraries, 03 medical and health sciences, Splicing factor, Stilbenes, Humans, lcsh:QH573-671, Cells, Cultured, Cellular Senescence, Cell Proliferation, lcsh:Cytology, Alternative splicing, Cell Cycle, Cell Biology, Cell cycle, Fibroblasts, Cell biology, Telomere, Ageing, Alternative Splicing, 030104 developmental biology, Resveratrol, RNA splicing, Research Article

Abstract

Background Altered expression of mRNA splicing factors occurs with ageing in vivo and is thought to be an ageing mechanism. The accumulation of senescent cells also occurs in vivo with advancing age and causes much degenerative age-related pathology. However, the relationship between these two processes is opaque. Accordingly we developed a novel panel of small molecules based on resveratrol, previously suggested to alter mRNA splicing, to determine whether altered splicing factor expression had potential to influence features of replicative senescence. Results Treatment with resveralogues was associated with altered splicing factor expression and rescue of multiple features of senescence. This rescue was independent of cell cycle traverse and also independent of SIRT1, SASP modulation or senolysis. Under growth permissive conditions, cells demonstrating restored splicing factor expression also demonstrated increased telomere length, re-entered cell cycle and resumed proliferation. These phenomena were also influenced by ERK antagonists and agonists. Conclusions This is the first demonstration that moderation of splicing factor levels is associated with reversal of cellular senescence in human primary fibroblasts. Small molecule modulators of such targets may therefore represent promising novel anti-degenerative therapies. Electronic supplementary material The online version of this article (10.1186/s12860-017-0147-7) contains supplementary material, which is available to authorized users.

Published

2020

29. FOXO1 and ETV6 genes may represent novel regulators of splicing factor expression in cellular senescence

Author

Elizabeth L. Ostler, Lorna W. Harries, Richard G. A. Faragher, and Eva Latorre

Subjects

0301 basic medicine, Senescence, Cell signaling, Cellular homeostasis, Biology, Biochemistry, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, Genetics, Humans, Phosphorylation, Molecular Biology, Protein kinase B, Cells, Cultured, Cellular Senescence, Cell Proliferation, Gene knockdown, Proto-Oncogene Proteins c-ets, Forkhead Box Protein O1, Alternative splicing, Fibroblasts, Cell biology, Repressor Proteins, 030104 developmental biology, RNA splicing, RNA Splicing Factors, Protein Kinases, 030217 neurology & neurosurgery, Signal Transduction, Biotechnology

Abstract

Cellular plasticity is a key facet of cellular homeostasis requiring correct temporal and spatial patterns of alternative splicing. Splicing factors, which orchestrate this process, demonstrate age-related dysregulation of expression; they are emerging as potential influences on aging and longevity. The upstream drivers of these alterations are still unclear but may involve aberrant cellular signaling. We compared the phosphorylation status of proteins in multiple signaling pathways in early and late passage human primary fibroblasts. We then assessed the impact of chemical inhibition or targeted knockdown of direct downstream targets of the ERK and AKT pathways on splicing factor expression, cellular senescence, and proliferation kinetics in senescent primary human fibroblasts. Components of the ERK and AKT signaling pathways demonstrated altered activation during cellular aging. Inhibition of AKT and ERK pathways led to up-regulation of splicing factor expression, reduction in senescent cell load, and partial reversal of multiple cellular senescence phenotypes in a dose-dependent manner. Furthermore, targeted knockdown of the genes encoding the downstream targets FOXO1 or ETV6 was sufficient to mimic these observations. Our results suggest that age-associated dysregulation of splicing factor expression and cellular senescence may derive in part from altered activity of ERK and AKT signaling and may act in part through the ETV6 and FOXO1 transcription factors. Targeting the activity of downstream effectors of ERK and AKT may therefore represent promising targets for future therapeutic intervention.-Latorre, E., Ostler, E. L., Faragher, R. G. A., Harries, L. W. FOXO1 and ETV6 genes may represent novel regulators of splicing factor expression in cellular senescence.

Published

2018

30. The Common HNF1A Variant I27L Is a Modifier of Age at Diabetes Diagnosis in Individuals With HNF1A-MODY

Author

Andrew R. Wood, Sian Ellard, Kashyap A. Patel, Christine Bellanné-Chantelot, Lorna W. Harries, Michael N. Weedon, Andrew T. Hattersley, Jonathan M. Locke, Cécile Saint-Martin, Seth A. Sharp, and Thomas W Laver

Subjects

0301 basic medicine, Oncology, endocrine system, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Genome-wide association study, Type 2 diabetes, medicine.disease, HNF1A, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Missense mutation, Age of onset, Allele, business, Allele frequency

Abstract

There is wide variation in the age at diagnosis of diabetes in individuals with maturity-onset diabetes of the young (MODY) due to a mutation in the HNF1A gene. We hypothesized that common variants at the HNF1A locus (rs1169288 [I27L], rs1800574 [A98V]), which are associated with type 2 diabetes susceptibility, may modify age at diabetes diagnosis in individuals with HNF1A-MODY. Meta-analysis of two independent cohorts, comprising 781 individuals with HNF1A-MODY, found no significant associations between genotype and age at diagnosis. However after stratifying according to type of mutation (protein-truncating variant [PTV] or missense), we found each 27L allele to be associated with a 1.6-year decrease (95% CI −2.6, −0.7) in age at diagnosis, specifically in the subset (n = 444) of individuals with a PTV. The effect size was similar and significant across the two independent cohorts of individuals with HNF1A-MODY. We report a robust genetic modifier of HNF1A-MODY age at diagnosis that further illustrates the strong effect of genetic variation within HNF1A upon diabetes phenotype.

Published

2018

31. Human longevity: 25 genetic loci associated in 389,166 UK biobank participants

Author

Luke C. Pilling, David Melzer, Lorna W. Harries, Pamela Herd, Jone Tamosauskaite, Robert B. Wallace, George A. Kuchel, Luigi Ferrucci, Chia-Ling Kuo, and Kamil Sicinski

Subjects

Adult, Male, Parents, 0301 basic medicine, Multifactorial Inheritance, Aging, Longitudinal study, media_common.quotation_subject, Longevity, Genome-wide association study, Disease, Biology, 03 medical and health sciences, 0302 clinical medicine, GWAS, Humans, human, Aged, Biological Specimen Banks, media_common, Cell Biology, Middle Aged, Health and Retirement Study, Biobank, United Kingdom, 3. Good health, 030104 developmental biology, Human longevity, Female, genetic, Centenarian, 030217 neurology & neurosurgery, Research Paper, Genome-Wide Association Study, Demography

Abstract

We undertook a genome-wide association study (GWAS) of parental longevity in European descent UK Biobank participants. For combined mothers' and fathers' attained age, 10 loci were associated (p

Published

2017

32. Splicing regulatory factors, ageing and age-related disease

Author

Eva Latorre and Lorna W. Harries

Subjects

0301 basic medicine, Gene isoform, Genetics, Aging, Alternative splicing, Regulator, Computational biology, Biology, Biochemistry, Alternative Splicing, 03 medical and health sciences, 030104 developmental biology, Neurology, Cardiovascular Diseases, Heterogeneous-Nuclear Ribonucleoprotein Group A-B, Gene expression, RNA splicing, Animals, Humans, RNA, Messenger, Molecular Biology, Gene, Function (biology), Biotechnology, Ribonucleoprotein

Abstract

Alternative splicing is a co-transcriptional process, which allows for the production of multiple transcripts from a single gene and is emerging as an important control point for gene expression. Alternatively expressed isoforms often have antagonistic function and differential temporal or spatial expression patterns, yielding enormous plasticity and adaptability to cells and increasing their ability to respond to environmental challenge. The regulation of alternative splicing is critical for numerous cellular functions in both pathological and physiological conditions, and deregulated alternative splicing is a key feature of common chronic diseases. Isoform choice is controlled by a battery of splicing regulatory proteins, which include the serine arginine rich (SRSF) proteins and the heterogeneous ribonucleoprotein (hnRNP) classes of genes. These important splicing regulators have been implicated in age-related disease, and in the ageing process itself. This review will outline the important contribution of splicing regulator proteins to ageing and age-related disease.

Published

2017

33. The inherent challenges of classifying senescence—Response

Author

Edward G. Lakatta, George M. Church, Cathy Slack, G. Alexander Fleming, Thomas J. Montine, Angelo Scuteri, Danica Chen, Claire E. Stewart, Arlan Richardson, Graham Pawelec, João Pedro de Magalhães, Michael J. Conboy, Lawrence Steinman, Karoly Nikolich, Clifford J. Rosen, Gary Marchant, Adam Antebi, Jesús Gil, Judith Campisi, Gary W. Small, Barry Bentley, Lorna W. Harries, Manlio Vinciguerra, Stuart R. G. Calimport, and Tony Wyss-Coray

Subjects

Senescence, Aging, Multidisciplinary, General Science & Technology, business.industry, Animals, Humans, Medicine, Cellular senescence, business, Cellular Senescence, Cell biology

Published

2020

34. Dietary restriction in ILSXISS mice is associated with widespread changes in splicing regulatory factor expression levels

Author

Colin Selman, Lorna W. Harries, Jemma Garratt, Gregory Barr, Benjamin P. Lee, Lorna Mulvey, and Emily Goodman

Subjects

0301 basic medicine, Aging, media_common.quotation_subject, Longevity, Biology, Health outcomes, Kidney, Biochemistry, law.invention, 03 medical and health sciences, Mice, 0302 clinical medicine, Endocrinology, Inbred strain, Species Specificity, law, Genetics, medicine, Tissue specific, Animals, Molecular Biology, media_common, Caloric Restriction, Strain (biology), Myocardium, Brain, Cell Biology, Alternative Splicing, 030104 developmental biology, medicine.anatomical_structure, Organ Specificity, RNA splicing, Recombinant DNA, 030217 neurology & neurosurgery

Abstract

Dietary restriction (DR) represents one of the most reproducible interventions to extend lifespan and improve health outcomes in a wide range of species, but substantial variability in DR response has been observed, both between and within species. The mechanisms underlying this variation in effect are still not well characterised. Splicing regulatory factors have been implicated in the pathways linked with DR-induced longevity in C. elegans and are associated with lifespan itself in mice and humans. We used qRT-PCR to measure the expression levels of a panel of 16 age- and lifespan-associated splicing regulatory factors in brain, heart and kidney derived from three recombinant inbred strains of mice with variable lifespan responses to short-term (2 months) or long-term (10 months) 40% DR to determine their relationship to DR-induced longevity. We identified 3 patterns of association; i) splicing factors associated with DR alone, ii) splicing factors associated with strain alone or iii) splicing factors associated with both DR and strain. Tissue specific variation was noted in response to short-term or long-term DR, with the majority of effects noted in brain following long-term DR in the positive responder strain TejJ89. Association in heart and kidney were less evident, and occurred following short-term DR. Splicing factors associated with both DR and strain may be mechanistically involved in strain-specific differences in response to DR. We provide here evidence concordant with a role for some splicing factors in the lifespan modulatory effects of DR across different mouse strains and in different tissues.

Published

2019

35. To help aging populations, classify organismal senescence

Author

Jesús Gil, Clifford J. Rosen, Gary Marchant, G. Alexander Fleming, Judith Campisi, Angelo Scuteri, Danica Chen, Adam Antebi, Arlan Richardson, Lorna W. Harries, Lawrence Steinman, George M. Church, Manlio Vinciguerra, Gary W. Small, Claire E. Stewart, Barry Bentley, Edward G. Lakatta, Graham Pawelec, Karoly Nikolich, Cathy Slack, Tony Wyss-Coray, Stuart R. G. Calimport, João Pedro de Magalhães, Thomas J. Montine, and Michael J. Conboy

Subjects

Senescence, Multidisciplinary, General Science & Technology, Cellular senescence, Disease classification, Biology, Bioinformatics

Abstract

Globally, citizens exist for sustained periods in states of aging-related disease and multimorbidity. Given the urgent and unmet clinical, health care, workforce, and economic needs of aging populations, we need interventions and programs that regenerate tissues and organs and prevent and reverse aging-related damage, disease, and frailty (1). In response to these challenges, the World Health Organization (WHO) has called for a comprehensive public-health response within an international legal framework based on human rights law (1). Yet for a clinical trial to be conducted, a disease to be diagnosed, intervention prescribed, and treatment administered; a corresponding disease classification code is needed, adopted nationally from the WHO International Classification of Diseases (ICD). Such classifications and staging are fundamental for health care governance among governments and intergovernmental bodies. We describe a systematic and comprehensive approach to the classification and staging of organismal senescence and aging-related diseases at the organ and tissue levels in order to guide policy and practice and enable appropriate interventions and clinical guidance, systems, resources, and infrastructure.

Published

2019

36. Author response: Androgen-regulated transcription of ESRP2 drives alternative splicing patterns in prostate cancer

Author

Bridget A. Knight, Nuno L. Barbosa-Morais, Mads Daugaard, Hanna A Zielinska, Ingrid Ehrmann, John J. McGrath, Oliver Thompson, Sebastian Oltean, Ling Li, Jennifer Munkley, Simon Cockell, Htoo Zarni Oo, Gerald Hysenaj, Lorna W. Harries, Kathleen Cheung, Emma Scott, David J. Elliott, Caroline Dalgliesh, Teresa Mendes Maia, S R Gokul Krishnan, Paul McCullagh, Karen E. Livermore, and Malcolm Crundwell

Subjects

Prostate cancer, medicine.drug_class, Transcription (biology), Alternative splicing, medicine, Cancer research, Biology, medicine.disease, Androgen

Published

2019

37. Astrocyte senescence may drive alterations in GFAPα, CDKN2A p14

Author

Jed J, Lye, Eva, Latorre, Ben P, Lee, Stefania, Bandinelli, Janet E, Holley, Nicholas J, Gutowski, Luigi, Ferrucci, and Lorna W, Harries

Subjects

Transcription, Genetic, Gene Expression, tau Proteins, Neurodegenerative disease, Senescence, Matrix Metalloproteinases, Alternative Splicing, Astrocytes, Glial Fibrillary Acidic Protein, Tumor Suppressor Protein p14ARF, Cytokines, Humans, Cognitive Dysfunction, Original Article, Cells, Cultured, Cellular Senescence, Aged

Abstract

The accumulation of senescent cells in tissues is causally linked to the development of several age-related diseases; the removal of senescent glial cells in animal models prevents Tau accumulation and cognitive decline. Senescent cells can arise through several distinct mechanisms; one such mechanism is dysregulation of alternative splicing. In this study, we characterised the senescent cell phenotype in primary human astrocytes in terms of SA-β-Gal staining and SASP secretion, and then assessed splicing factor expression and candidate gene splicing patterns. Finally, we assessed associations between expression of dysregulated isoforms and premature cognitive decline in 197 samples from the InCHIANTI study of ageing, where expression was present in both blood and brain. We demonstrate here that senescent astrocytes secrete a modified SASP characterised by increased IL8, MMP3, MMP10, and TIMP2 but decreased IL10 levels. We identified significant changes in splicing factor expression for 10/20 splicing factors tested in senescent astrocytes compared with early passage cells, as well as dysregulation of isoform levels for 8/13 brain or senescence genes tested. Finally, associations were identified between peripheral blood GFAPα, TAU3, and CDKN2A (P14ARF) isoform levels and mild or severe cognitive decline over a 3–7-year period. Our data are suggestive that some of the features of cognitive decline may arise from dysregulated splicing of important genes in senescent brain support cells, and that defects in alternative splicing or splicing regulator expression deserve exploration as points of therapeutic intervention in the future.

Published

2019

38. Alternative splicing in serotonergic system: Implications in neuropsychiatric disorders

Author

Eva Latorre, Lorna W. Harries, and José E. Mesonero

Subjects

Pharmacology, 0303 health sciences, Serotonin, Mental Disorders, Alternative splicing, Cell Plasticity, Biology, Serotonergic, 03 medical and health sciences, Psychiatry and Mental health, Alternative Splicing, 0302 clinical medicine, Gene Expression Regulation, Component (UML), Animals, Humans, Pharmacology (medical), RNA, Messenger, Nervous System Diseases, Neuroscience, 030217 neurology & neurosurgery, Brain function, 030304 developmental biology, Signal Transduction

Abstract

Background:The serotonergic system is a key component of physiological brain function and is essential for proper neurological activity. Numerous neuropsychiatric disorders are associated with deregulation of the serotonergic system. Accordingly, many pharmacological treatments are focused on modulation of this system. While providing a promising line of therapeutic moderation, these approaches may be complicated due to the presence of alternative splicing events for key genes in this pathway. Alternative splicing is a co-transcriptional process by which different mRNA transcripts can be produced from the same gene. These different isoforms may have diverse activities and functions, and their relative balance is often critical for the maintenance of homeostasis. Alternative splicing greatly increases the production of proteins, augmenting cell plasticity, and provides an important control point for regulation of gene expression.Aim:The objective of this narrative review is to discuss the potential impact of alternative splicing of different components of the serotonergic system and speculate on their involvement in several neuropsychiatric disorders.Conclusions:The specific role of each isoform in disease and their relative activities in the signalling pathways involved are yet to be determined. We need to gain a better understanding of the basis of alternative isoforms of the serotonergic system in order to fully understand their impact and be able to develop new effective pharmacological isoform-specific targets.

Published

2019

39. miRNAs responsive to the diabetic microenvironment in the human beta cell line EndoC-βH1 may target genes in the FOXO, HIPPO and Lysine degradation pathways

Author

Lorna W. Harries and Nicola Jeffery

Subjects

0301 basic medicine, Cell Survival, FOXO1, Biology, Protein Serine-Threonine Kinases, Cell Line, Fight-or-flight response, 03 medical and health sciences, 0302 clinical medicine, Insulin-Secreting Cells, microRNA, medicine, Diabetes Mellitus, Humans, Gene Regulatory Networks, Hippo Signaling Pathway, Gene, geography, geography.geographical_feature_category, Lysine degradation, Forkhead Box Protein O1, Gene Expression Profiling, Lysine, Cell Biology, Hypoxia (medical), Islet, Cell biology, MicroRNAs, 030104 developmental biology, Gene Ontology, Cellular Microenvironment, 030220 oncology & carcinogenesis, medicine.symptom, Beta cell

Abstract

Altered expression of miRNAs is evident in the islets of diabetic human donors, but the effects of specific aspects of the diabetic microenvironment and identity of gene ontology pathways demonstrating target gene enrichment in response to each is understudied. We assessed changes in the miRNA milieu in response to high/low glucose, hypoxia, dyslipidaemia and inflammatory factors in a humanised EndoC-βH1 beta cell culture system and performed miRPath analysis for each treatment individually. The 10 miRNAs demonstrating the greatest dysregulation across treatments were then independently validated and Gene Set Enrichment Analysis to confirm targeted pathways undertaken. 171 of 392 miRNAs displayed altered expression in response to one or more cellular stressors. miRNA changes were treatment specific, but their target genes were enriched in conserved pathways. 5 miRNAs (miR-136-5p, miR299-5p, miR-454-5p, miR-152 and miR-185) were dysregulated in response to multiple stressors and survived validation in independent samples (p = 0.008, 0.002, 0.012, 0.005 and 0.024 respectively). Target genes of dysregulated miRNAs were clustered into FOXO1, HIPPO and Lysine degradation pathways (p = 0.02, p = 5.84 × 10−5 and p = 3.00 × 10−3 respectively). We provide evidence that the diabetic microenvironment may induce changes to the expression of miRNAs targeting genes enriched in pathways involved in cell stress response and cell survival.

Published

2019

40. The transcript expression levels of HNRNPM, HNRNPA0 and AKAP17A splicing factors may be predictively associated with ageing phenotypes in human peripheral blood

Author

Stefania Bandinelli, David Melzer, Luigi Ferrucci, Luke C. Pilling, Lorna W. Harries, and Benjamin P. Lee

Subjects

0301 basic medicine, Male, Aging, Trail Making Test, Population, Cognitive decline, Biology, Bioinformatics, Heterogeneous-Nuclear Ribonucleoproteins, Splicing factors, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, Predictive Value of Tests, Purdue Pegboard Test, Humans, Cognitive Dysfunction, Antigens, education, Correlation of Data, Cellular Senescence, Aged, education.field_of_study, Membrane Glycoproteins, Hand Strength, Physical Functional Performance, Mental Status and Dementia Tests, Phenotype, Heterogeneous-Nuclear Ribonucleoprotein Group M, Walking Speed, 030104 developmental biology, Ageing, RNA splicing, Female, RNA Splicing Factors, Geriatrics and Gerontology, Gerontology, 030217 neurology & neurosurgery, Biomarkers, Research Article

Abstract

Dysregulation of splicing factor expression is emerging as a driver of human ageing; levels of transcripts encoding splicing regulators have previously been implicated in ageing and cellular senescence both in vitro and in vivo. We measured the expression levels of an a priori panel of 20 age- or senescence-associated splicing factors by qRT-PCR in peripheral blood samples from the InCHIANTI Study of Aging, and assessed longitudinal relationships with human ageing phenotypes (cognitive decline and physical ability) using multivariate linear regression. AKAP17A, HNRNPA0 and HNRNPM transcript levels were all predictively associated with severe decline in MMSE score (p = 0.007, 0.001 and 0.008 respectively). Further analyses also found expression of these genes was associated with a performance decline in two other cognitive measures; the Trail Making Test and the Purdue Pegboard Test. AKAP17A was nominally associated with a decline in mean hand-grip strength (p = 0.023), and further analyses found nominal associations with two other physical ability measures; the Epidemiologic Studies of the Elderly-Short Physical Performance Battery and calculated speed (m/s) during a timed 400 m fast walking test. These data add weight to the hypothesis that splicing dyregulation may contribute to the development of some ageing phenotypes in the human population. Electronic supplementary material The online version of this article (10.1007/s10522-019-09819-0) contains supplementary material, which is available to authorized users.

Published

2019

41. Androgen-regulated transcription ofESRP2drives alternative splicing patterns in prostate cancer

Author

Paul McCullagh, Emma Scott, David J. Elliott, Mads Daugaard, Oliver Thompson, John A. McGrath, Jennifer Munkley, Htoo Zarni Oo, Simon Cockell, Lorna W. Harries, Kathleen Cheung, Bridget A. Knight, Sebastian Oltean, Nuno L. Barbosa-Morais, Hanna A Zielinska, Karen E. Livermore, Gerald Hysenaj, Ingrid Ehrmann, Malcolm Crundwell, Teresa Mendes Maia, S R Gokul Krishnan, and Ling Li

Subjects

0303 health sciences, Bicalutamide, medicine.drug_class, Alternative splicing, Biology, medicine.disease, Androgen, Metastasis, Androgen receptor, Androgen deprivation therapy, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, 030220 oncology & carcinogenesis, RNA splicing, medicine, Cancer research, 030304 developmental biology, medicine.drug

Abstract

Prostate is the most frequent cancer in men. Prostate cancer progression is driven by androgen steroid hormones, and delayed by androgen deprivation therapy (ADT). Androgens control transcription by stimulating androgen receptor (AR) activity, yet also control pre-mRNA splicing through less clear mechanisms. Here we find androgens regulate splicing through AR-mediated transcriptional control of the epithelial-specific splicing regulatorESRP2. BothESRP2and its close paralogESRP1are highly expressed in primary prostate cancer. Androgen stimulation induces splicing switches in many endogenous ESRP2-controlled mRNA isoforms, including a key splicing switch in the metastatic regulatorFLNBwhich is associated with disease relapse.ESRP2expression in clinical prostate cancer is repressed by ADT, which may thus inadvertently dampen epithelial splice programmes. Supporting this,FLNBsplicing was reciprocally switched by the AR antagonist bicalutamide (Casodex®). Our data reveal a new mechanism of splicing control in prostate cancer with important implications for metastatic disease progression.Key pointsTranscriptional regulation of ESRP2 by the androgen receptor controls splice isoform patterns in prostate cancer cells.Splicing switches regulated by the androgen-ESRP2 axis include a splice isoform in theFLNBgene that is a known metastatic driver.Both ESRP1 and ESRP2 are highly expressed in prostate cancer tissue.Ectopic expression of ESRP1 and 2 inhibits prostate cancer cell growth.By repressing ESRP2 expression androgen deprivation therapy (ADT) may dampen epithelial splicing programmes to inadvertently prime disease progression towards metastasis.

Published

2019

42. Obesity impacts the regulation of miR-10b and its targets in primary breast tumors

Author

Bridget A. Knight, Hila Yehuda, Malcolm Crundwell, Ari Meerson, Lorna W. Harries, Yaniv Eliraz, Douglas Ferguson, and Benjamin P. Lee

Subjects

Adult, 0301 basic medicine, Cancer Research, Tumor suppressors, Down-Regulation, Breast Neoplasms, lcsh:RC254-282, 03 medical and health sciences, Breast cancer, 0302 clinical medicine, CDKN2A, Surgical oncology, microRNA, Tumor Cells, Cultured, Genetics, Humans, Medicine, Obesity, Gene, Aged, Aged, 80 and over, business.industry, Cell growth, Gene Expression Profiling, Cancer, Oncogenes, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Prognosis, medicine.disease, 3. Good health, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, Oncology, BCL2L11, 030220 oncology & carcinogenesis, Cancer research, Female, business, miR-10b, Research Article

Abstract

Background Obesity increases breast cancer (BC) risk in post-menopausal women by mostly unknown molecular mechanisms which may partly be regulated by microRNAs (miRNAs). Methods We isolated RNA from paired benign and malignant biopsies from 83 BC patients and determined miRNA profiles in samples from 12 women at the extremes of the BMI distribution by RNA-seq. Candidates were validated in all samples. Associations between miR-10b expression and validated target transcript levels, and effects of targeted manipulation of miR-10b levels in a primary BC cell line on proliferation and invasion potential, were explored. Results Of the 148 miRNAs robustly expressed in breast tissues, the levels of miR-21, miR-10b, miR-451a, miR-30c, and miR-378d were significantly associated with presence of cancer. Of these, miR-10b showed a stronger down-regulation in the tumors of the obese subjects, as opposed to the lean. In ductal but not lobular tumors, significant inverse correlations were observed between the tumor levels of miR-10b and miR-30c and the mRNA levels of cancer-relevant target genes SRSF1, PIEZO1, MAPRE1, CDKN2A, TP-53 and TRA2B, as well as tumor grade. Suppression of miR-10b levels in BT-549 primary BC–derived cells increased cell proliferation and invasive capacity, while exogenous miR-10b mimic decreased invasion. Manipulation of miR-10b levels also inversely affected the mRNA levels of miR-10b targets BCL2L11, PIEZO1 and NCOR2. Conclusions Our findings suggest that miR-10b may be a mediator between obesity and cancer in post-menopausal women, regulating several known cancer-relevant genes. MiR-10b expression may have diagnostic and therapeutic implications for the incidence and prognosis of BC in obese women. Electronic supplementary material The online version of this article (10.1186/s12885-019-5300-6) contains supplementary material, which is available to authorized users.

Published

2019

43. β-cell differentiation status in type 2 diabetes

Author

Lorna W. Harries and Nicola Jeffery

Subjects

0301 basic medicine, medicine.medical_specialty, endocrine system diseases, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Cellular differentiation, Apoptosis, Disease, Type 2 diabetes, Bioinformatics, Epigenesis, Genetic, 03 medical and health sciences, Endocrinology, Insulin resistance, Insulin-Secreting Cells, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Animals, Humans, Epigenetics, Hypoxia, Loss function, Inflammation, business.industry, Insulin, nutritional and metabolic diseases, Cell Differentiation, Cell Dedifferentiation, medicine.disease, 030104 developmental biology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Hyperglycemia, business, Transcription Factors

Abstract

Type 2 diabetes (T2D) affects 415 million people worldwide and is characterized by chronic hyperglycaemia and insulin resistance, progressing to insufficient insulin production, as a result of β-cell failure. Over time, chronic hyperglycaemia can ultimately lead to loss of β-cell function, leaving patients insulin-dependent. Until recently the loss of β-cell mass seen in T2D was considered to be the result of increased rates of apoptosis; however, it has been proposed that apoptosis alone cannot account for the extent of β-cell mass loss seen in the disease, and that a loss of function may also occur as a result of changes in β-cell differentiation status. In the present review, we consider current knowledge of determinants of β-cell fate in the context of understanding its relevance to disease process in T2D, and also the impact of a diabetogenic environment (hyperglycaemia, hypoxia, inflammation and dyslipidaemia) on the expression of genes involved in maintenance of β-cell identity. We describe current knowledge of the impact of the diabetic microenvironment on gene regulatory processes such alternative splicing, the expression of disallowed genes and epigenetic modifications. Elucidating the molecular mechanisms that underpin changes to β-cell differentiation status and the concomitant β-cell failure offers potential treatment targets for the future management of patients with T2D.

Published

2016

44. Functional characterisation of ADIPOQ variants using individuals recruited by genotype

Author

Giles O. Cory, Henry O. Lloyd-Laney, Lorna W. Harries, Hanieh Yaghootkar, Katarina Kos, Bridget A. Knight, Benjamin P. Lee, Jonathan M. Locke, Timothy M. Frayling, and Laura J. McCulloch

Subjects

Male, 0301 basic medicine, Genotype, RNA Splicing, Genome-wide association study, Biology, ADIPOQ Gene, Polymorphism, Single Nucleotide, Biochemistry, 03 medical and health sciences, Endocrinology, Gene Frequency, RNA Precursors, Humans, RNA, Messenger, Allele, Molecular Biology, Allele frequency, Alleles, Genetics, Regulation of gene expression, Base Sequence, 030102 biochemistry & molecular biology, Adiponectin, Computational Biology, Middle Aged, 030104 developmental biology, Adipose Tissue, Gene Expression Regulation, RNA splicing, Female, RNA, Long Noncoding

Abstract

Four non-coding GWAS variants in or near the ADIPOQ gene (rs17300539, rs17366653, rs3821799 and rs56354395) together explain 4% of the variation in circulating adiponectin. The functional basis for this is unknown. We tested the effect of these variants on ADIPOQ transcription, splicing and stability respectively in adipose tissue samples from participants recruited by rs17366653 genotype. Transcripts carrying rs17300539 demonstrated a 17% increase in expression (p = 0.001). Variant rs17366653 was associated with disruption of ADIPOQ splicing leading to a 7 fold increase in levels of a non-functional transcript (p = 0.002). Transcripts carrying rs56354395 demonstrated a 59% decrease in expression (p =

Published

2016

45. Peripheral Blood Transcriptomic Signatures of Fasting Glucose and Insulin Concentrations

Author

Joyce B. J. van Meurs, Eric D. Kolaczyk, Roby Joehanes, Caroline S. Fox, Albert Hofman, Andrew B. Singleton, Jose C. Florez, Andrew D. Johnson, Denis Rybin, Magic Investigators, Jaeyoung Hong, Lorna W. Harries, Lisa Pham, James B. Meigs, André G. Uitterlinden, Daniel Levy, Josée Dupuis, Stefania Bandinelli, Marie-France Hivert, Luigi Ferrucci, Dena G. Hernandez, Luke C. Pilling, Marjolein J. Peters, Brian H. Chen, Peter J. Munson, Abbas Dehghan, John D. Hogan, Saixia Ying, David Melzer, Internal Medicine, and Epidemiology

Subjects

0301 basic medicine, Adult, Blood Glucose, Male, medicine.medical_specialty, Genotype, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Quantitative Trait Loci, 030209 endocrinology & metabolism, Genome-wide association study, Biology, 03 medical and health sciences, Rotterdam Study, 0302 clinical medicine, Framingham Heart Study, Diabetes mellitus, Internal medicine, Internal Medicine, medicine, Humans, Insulin, Genetic Predisposition to Disease, RNA, Messenger, Allele, Glycemic, Aged, RNA-Binding Proteins, Genetics/Genomes/Proteomics/Metabolomics, Fasting, Middle Aged, medicine.disease, 030104 developmental biology, Endocrinology, Expression quantitative trait loci, Female, Transcriptome, Genome-Wide Association Study

Abstract

Genome-wide association studies (GWAS) have successfully identified genetic loci associated with glycemic traits. However, characterizing the functional significance of these loci has proven challenging. We sought to gain insights into the regulation of fasting insulin and fasting glucose through the use of gene expression microarray data from peripheral blood samples of participants without diabetes in the Framingham Heart Study (FHS) (n = 5,056), the Rotterdam Study (RS) (n = 723), and the InCHIANTI Study (Invecchiare in Chianti) (n = 595). Using a false discovery rate q

Published

2016

46. Physiological effects of Type 2 diabetes on mRNA processing and gene expression

Author

Karen A. Johnstone, Lorna W. Harries, and Faer S Morrison

Subjects

Regulation of gene expression, medicine.medical_specialty, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Alternative splicing, nutritional and metabolic diseases, Type 2 diabetes, Biology, medicine.disease, Endocrinology, Internal medicine, Diabetes mellitus, microRNA, Gene expression, Hyperlipidemia, medicine, Epigenetics

Abstract

Characteristics of Type 2 diabetes include both high blood glucose (hyperglycemia) and raised cholesterol and triglycerides (hyperlipidemia). Several studies have now shown that both hyperglycemia and hyperlipidemia can alter gene expression by disrupting physiological mechanisms of gene regulation, including alternative mRNA splicing, epigenetic gene regulation and miRNA-mediated regulation of gene expression. These processes may also be influenced by intracellular oxidative stress, which is increased in diabetes and in response to hyperglycemia and hyperlipidemia. Many pathways relevant to diabetes are affected by altered gene expression, including lipid and glucose metabolism and oxidative phosphorylation. This article considers how hyperglycemia and hyperlipidemia can alter gene expression in diabetes, which could potentially contribute to the worsening of the diabetic phenotype and diabetic complications.

Published

2018

47. Altered cellular redox homeostasis and redox responses under standard oxygen cell culture conditions versus physioxia

Author

Daniel C J, Ferguson, Gary R, Smerdon, Lorna W, Harries, Nicholas J F, Dodd, Michael P, Murphy, Alison, Curnow, and Paul G, Winyard

Subjects

Oxygen, Photochemotherapy, Cell Culture Techniques, Animals, Homeostasis, Humans, Hyperoxia, Reactive Oxygen Species, Oxidation-Reduction, Metabolic Networks and Pathways, Mitochondria

Abstract

In vivo, mammalian cells reside in an environment of 0.5-10% O

Published

2018

48. Mitochondria-targeted hydrogen sulfide attenuates endothelial senescence by selective induction of splicing factors

Author

Eva, Latorre, Roberta, Torregrossa, Mark E, Wood, Matthew, Whiteman, and Lorna W, Harries

Subjects

senescence, persulfide, Serine-Arginine Splicing Factors, H2S, Morpholines, Thiones, Epithelial Cells, Organothiophosphorus Compounds, AP39, Cell Line, Organophosphorus Compounds, Gene Expression Regulation, splicing factors, RT01, mitochondria-targeting, Humans, perthiol, Heterogeneous Nuclear Ribonucleoprotein D0, Hydrogen Sulfide, RNA Splicing Factors, Heterogeneous-Nuclear Ribonucleoprotein D, Transcriptome, AP123, Cellular Senescence, Research Paper

Abstract

Cellular senescence is a key driver of ageing, influenced by age-related changes to the regulation of alternative splicing. Hydrogen sulfide (H2S) has similarly been described to influence senescence, but the pathways by which it accomplishes this are unclear. We assessed the effects of the slow release H2S donor Na-GYY4137 (100 µg/ml), and three novel mitochondria-targeted H2S donors AP39, AP123 and RT01 (10 ng/ml) on splicing factor expression, cell proliferation, apoptosis, DNA replication, DNA damage, telomere length and senescence-related secretory complex (SASP) expression in senescent primary human endothelial cells. All H2S donors produced up to a 50% drop in senescent cell load assessed at the biochemical and molecular level. Some changes were noted in the composition of senescence-related secretory complex (SASP); IL8 levels increased by 24% but proliferation was not re-established in the culture as a whole. Telomere length, apoptotic index and the extent of DNA damage were unaffected. Differential effects on splicing factor expression were observed depending on the intracellular targeting of the H2S donors. Na-GYY4137 produced a general 1.9 – 3.2-fold upregulation of splicing factor expression, whereas the mitochondria-targeted donors produced a specific 2.5 and 3.1-fold upregulation of SRSF2 and HNRNPD splicing factors only. Knockdown of SRSF2 or HNRNPD genes in treated cells rendered the cells non-responsive to H2S, and increased levels of senescence by up to 25% in untreated cells. Our data suggest that SRSF2 and HNRNPD may be implicated in endothelial cell senescence, and can be targeted by exogenous H2S. These molecules may have potential as moderators of splicing factor expression and senescence phenotypes.

Published

2018

49. The VEGFA156b isoform is dysregulated in senescent endothelial cells and may be associated with prevalent and incident coronary heart disease

Author

Benjamin P. Lee, Lorna W. Harries, Luigi Ferrucci, David Melzer, Eva Latorre, Luke C. Pilling, and Stefania Bandinelli

Subjects

0301 basic medicine, Senescence, Vascular Endothelial Growth Factor A, medicine.medical_specialty, Cell type, Candidate gene, Population, Coronary Disease, Article, Coronary artery disease, 03 medical and health sciences, Splicing factor, Internal medicine, medicine, Humans, Protein Isoforms, RNA, Small Interfering, education, Cells, Cultured, Cellular Senescence, education.field_of_study, business.industry, Incidence, Alternative splicing, Endothelial Cells, General Medicine, medicine.disease, Alternative Splicing, 030104 developmental biology, Endocrinology, RNA splicing, Endothelium, Vascular, business

Abstract

Coronary heart disease (CHD) is a leading cause of morbidity in people over 65 years of age; >40% of all deaths are due to this condition. The association between increasing age and CHD is well documented; the accumulation of senescent cells in cardiac and vascular tissues may represent one factor underpinning this observation. We aimed to identify senescence-related expression changes in primary human senescent cardiomyocytes and endothelial cells and to relate transcript expression in peripheral blood leucocytes to prevalent and incident CHD in the InCHIANTI study of aging. We quantified splicing factor expression and splicing patterns of candidate transcripts in proliferative and senescent later passage endothelial cells and cardiomyocytes using qRTPCR. Senescence-associated isoforms also expressed in peripheral blood leucocytes were then examined for associations with CHD status in 134 pairs of age, sex and BMI-matched CHD cases and controls. Splicing factor expression was dysregulated in senescent cardiomyocytes, as previously reported for endothelial cells, as was the expression of alternatively expressed cardiac and vascular candidate genes in both cell types. We found nominal associations between the expression of VEGFA156b and FNI-EIIIIA isoforms in peripheral blood mRNA and CHD status. Dysregulated splicing factor expression is a key feature of senescent cardiomyocytes and endothelial cells. Altered splicing of key cardiac or endothelial genes may contribute to the risk of CHD in the human population.

Published

2018

50. Comparison of senescence-associated miRNAs in primary skin and lung fibroblasts

Author

Luke C. Pilling, Luigi Ferrucci, Pieter Van de Walle, Lorna W. Harries, David Dolan, Sushma Nagaraja Grellscheid, David Melzer, Thomas von Zglinicki, Alice C. Holly, and Darren J. Daniels

Subjects

Senescence, Aging, Pathology, medicine.medical_specialty, Cell type, Time Factors, Cell, Biology, Article, Cell Line, microRNA, medicine, Humans, Lung, Cellular Senescence, Cell Proliferation, Skin, Regulation of gene expression, Gene Expression Profiling, Age Factors, Computational Biology, Fibroblasts, Gene expression profiling, MicroRNAs, medicine.anatomical_structure, Gene Expression Regulation, Cell culture, Cancer research, Geriatrics and Gerontology, Gerontology, Cell aging

Abstract

MicroRNAs are non-coding RNAs with roles in many cellular processes. Tissue-specific miRNA profiles associated with senescence have been described for several cell and tissue types. We aimed to characterise miRNAs involved in core, rather than tissue-specific, senescence pathways by assessment of common miRNA expression differences in two different cell types, with follow-up of predicted targets in human peripheral blood. MicroRNAs were profiled in early and late passage primary lung and skin fibroblasts to identify commonly-deregulated miRNAs. Expression changes of their bioinformatically-predicted mRNA targets were then assessed in both cell types and in human peripheral blood from elderly participants in the InCHIANTI study. 57/178 and 26/492 microRNAs were altered in late passage skin and lung cells respectively. Three miRNAs (miR-92a, miR-15b and miR-125a-3p) were altered in both tissues. 14 mRNA targets of the common miRNAs were expressed in lung and skin fibroblasts, of which two demonstrated up-regulation in late passage skin and lung cells (LYST; p = 0.02 [skin] and 0.02 [lung] INMT; p = 0.03 [skin] and 0.04 [lung]). ZMPSTE24 and LHFPL2 demonstrated altered expression in late passage skin cells only (p = 0.01 and 0.05 respectively). LHFPL2 was also positively correlated with age in peripheral blood (p value = 6.6 × 10(-5)). We find that the majority of senescence-associated miRNAs demonstrate tissue-specific effects. However, miRNAs showing common effects across tissue types may represent those associated with core, rather than tissue-specific senescence processes.

Published

2015