Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

Benyelles, Maname; Episkopou, Harikleia; O’Donohue, Marie-Françoise; Kermasson, Laëtitia; Frange, Pierre; Poulain, Florian; Belen, Fatma Burcu; Polat, Meltem; Bôle‐Feysot, Christine; Langa‐Vives, Francina; Gleizes, Pierre‐Emmanuel; Villartay, Jean‐Pierre de; Callebaut, Isabelle; Decottignies, Anabelle; Revy, Patrick

doi:10.15252/emmm.201810201

Cited by 34 publications

(43 citation statements)

References 56 publications

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“…More recently, it was found that PARN directly trims rRNA precursors and that RNAi depletion of PARN causes their accumulation (Montellese et al, ). In addition, while this manuscript was in revision, Benyelles et al () reported accumulation of 18S pre‐rRNAs in samples derived from HH individuals, as we do here in our proband (Figure d–f), and in a cell line with biallelic PARN knockout. Interestingly, we observed that neither cells with a knockout of a single allele (Figure g) nor individuals heterozygous for pathogenic PARN variants (Figure d–f) had an accumulation of 18S pre‐rRNA, suggesting a dose‐dependent effect.…”

Section: Discussionsupporting

confidence: 73%

“…Nonetheless, telomeres shortened. It is possible that monoallelic loss of PARN causes telomere shortening through an RNA other than hTR in HCT116 cells, such as that encoding TPP1, as observed in PARN‐deficient HT1080 cells (Benyelles et al, ) or that increased hTR adenylation is sufficient to shorten telomeres.…”

Section: Discussionmentioning

confidence: 99%

“…Subsequently, patients with biallelic variants in PARN were identified in a cohort of patients with HH (Tummala et al, ). To date, greater than 50 cases with IPF, eight cases with HH, and three cases with DC, have been reported with PARN as the underlying etiology (Alder et al, ; Benyelles et al, ; Burris et al, ; Dhanraj et al, ; Kropski et al, ; Moon et al, ; Newton et al, ; Petrovski et al, ; Tummala et al, ). The phenomenon of monoallelic variants causing adult‐onset IPF and biallelic variants causing a pediatric TBD has also been observed for TERT and RTEL1 (Armanios et al, ; Ballew, Joseph, et al, ; Ballew, Yeager, et al, ; Deng et al, ; Gramatges, Qi, Sasa, Chen, & Bertuch, ; Kannengiesser et al, ; Le Guen et al, ; Marrone et al, ; Stuart et al, ; Tsakiri et al, ; Walne, Vulliamy, Kirwan, Plagnol, & Dokal, ).…”

Section: Introductionmentioning

confidence: 99%

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From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

et al. 2019

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PARN encodes poly(A)-specific ribonuclease. Biallelic and monoallelic PARN variants are associated with Hoyeraal-Hreidarsson syndrome/dyskeratosis congenita and idiopathic pulmonary fibrosis (IPF), respectively. The molecular features associated with incomplete penetrance of PARN-associated IPF have not been described. We report a family with a rare missense, p.Y91C, and a novel insertion, p.(I274*), PARN variant. We found PARN p.Y91C had reduced deadenylase activity and the p.(I274*) transcript was depleted. Detailed analysis of the consequences of these variants revealed that, while PARN protein was lowest in the severely affected biallelic child who had the shortest telomeres, it was also reduced in his mother with the p.(I274*) variant but telomeres at the 50th percentile. Increased adenylation of telomerase RNA, human telomerase RNA, and certain small nucleolar RNAs, and impaired ribosomal RNA maturation were observed in cells derived from the severely affected biallelic carrier, but not in the other, less affected biallelic carrier, who had less severely shortened telomeres, nor in the monoallelic carriers who were unaffected and had telomeres ranging from the 1st to the 50th percentiles. We identified hsa-miR-202-5p as a potential negative regulator of PARN. We propose one or more genetic modifiers influence the impact of PARN variants on its targets and this underlies incomplete penetrance of PARN-associated disease. K E Y W O R D S idiopathic pulmonary fibrosis, incomplete penetrance, MIR202, PARN, poly(A)-specific ribonuclease, telomere biology disorder

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Section: Discussionsupporting

confidence: 73%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

et al. 2019

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“…This mutation is located in the β‐fold region of PARN (Figure 3A), predicted to lead to the loss of a hydrogen bond in the protein structure and is highly conserved in all 14 species (Figure 3B,F). The pathogenicity of the biallele mutation at this locus has been demonstrated in a Hoyeraal‐Hreidarsson patient reported by Benyelles 23 . Considering P1 also showed the manifestations of Hoyeraal‐Hreidarsson syndrome, we performed direct sequencing of the full PARN coding sequence in P1 and his parents.…”

Section: Resultsmentioning

confidence: 99%

CD8⁺ T‐cell senescence and skewed lymphocyte subsets in young Dyskeratosis Congenita patients with PARN and DKC1 mutations

Zeng

Lü

et al. 2020

Clinical Laboratory Analysis

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Background Dyskeratosis congenita (DC) is a syndrome resulting from defective telomere maintenance. Immunodeficiency associated with DC can cause significant morbidity and lead to premature mortality, but the immunological characteristics and molecular hallmark of DC patients, especially young patients, have not been described in detail. Methods We summarize the clinical data of two juvenile patients with DC. Gene mutations were identified by whole‐exome and direct sequencing. Swiss‐PdbViewer was used to predict the pathogenicity of identified mutations. The relative telomere length was determined by QPCR, and a comprehensive analysis of lymphocyte subsets and CD57 expression was performed by flow cytometry. Results Both patients showed typical features of DC without severe infection. In addition, patient 1 (P1) was diagnosed with Hoyeraal‐Hreidarsson syndrome due to cerebellar hypoplasia. Gene sequencing showed P1 had a compound heterozygous mutation (c.204G > T and c.178‐245del) in PARN and P2 had a novel hemizygous mutation in DKC1 (c.1051A > G). Lymphocyte subset analysis showed B and NK cytopenia, an inverted CD4:CD8 ratio, and decreased naïve CD4 and CD8 cells. A significant increase in CD21low B cells and skewed numbers of helper T cells (Th), regulatory T cells (Treg), follicular regulatory T cells (Tfr), and follicular helper T cells (Tfh) were also detected. Short telomere lengths, increased CD57 expression, and an expansion of CD8 effector memory T cells re‐expressing CD45RA (TEMRA) were also found in both patients. Conclusion Unique immunologic abnormalities, CD8 T‐cell senescence, and shortened telomere together as a hallmark occur in young DC patients before progression to severe disease.

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“…While the investigated patient cells also show genome-wide damage, this damage is apparently tolerable when telomeres are sufficiently long and in itself does not cause a significant cell growth defects. Dyskerin, PARN and TCAB1/WRAP53β are involved in various pathways other than telomerase action, such as rRNA modification and biogenesis, mRNA stability, DDR and scaRNAs trafficking to the Cajal bodies ( 46–48 ). In the context of TBD, however, point mutations in these genes are all associated with the common phenotype of reduced telomerase action.…”

Section: Discussionmentioning

confidence: 99%

Full length RTEL1 is required for the elongation of the single-stranded telomeric overhang by telomerase

Awad

Glousker

Lamm

et al. 2020

Nucleic Acids Research

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Telomeres cap the ends of eukaryotic chromosomes and distinguish them from broken DNA ends to suppress DNA damage response, cell cycle arrest and genomic instability. Telomeres are elongated by telomerase to compensate for incomplete replication and nuclease degradation and to extend the proliferation potential of germ and stem cells and most cancers. However, telomeres in somatic cells gradually shorten with age, ultimately leading to cellular senescence. Hoyeraal-Hreidarsson syndrome (HHS) is characterized by accelerated telomere shortening and diverse symptoms including bone marrow failure, immunodeficiency, and neurodevelopmental defects. HHS is caused by germline mutations in telomerase subunits, factors essential for its biogenesis and recruitment to telomeres, and in the helicase RTEL1. While diverse phenotypes were associated with RTEL1 deficiency, the telomeric role of RTEL1 affected in HHS is yet unknown. Inducible ectopic expression of wild-type RTEL1 in patient fibroblasts rescued the cells, enabled telomerase-dependent telomere elongation and suppressed the abnormal cellular phenotypes, while silencing its expression resulted in gradual telomere shortening. Our observations reveal an essential role of the RTEL1 C-terminus in facilitating telomerase action at the telomeric 3′ overhang. Thus, the common etiology for HHS is the compromised telomerase action, resulting in telomere shortening and reduced lifespan of telomerase positive cells.

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Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

Cited by 34 publications

References 56 publications

From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

CD8⁺ T‐cell senescence and skewed lymphocyte subsets in young Dyskeratosis Congenita patients with PARN and DKC1 mutations

Full length RTEL1 is required for the elongation of the single-stranded telomeric overhang by telomerase

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Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

Cited by 34 publications

References 56 publications

From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

From incomplete penetrance with normal telomere length to severe disease and telomere shortening in a family with monoallelic and biallelic PARN pathogenic variants

CD8+ T‐cell senescence and skewed lymphocyte subsets in young Dyskeratosis Congenita patients with PARN and DKC1 mutations

Full length RTEL1 is required for the elongation of the single-stranded telomeric overhang by telomerase

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CD8⁺ T‐cell senescence and skewed lymphocyte subsets in young Dyskeratosis Congenita patients with PARN and DKC1 mutations