<scp><i>TAF1</i></scp> Transcripts and Neurofilament Light Chain as Biomarkers for X‐linked Dystonia‐Parkinsonism

Ali, Jamal Al; Vaine, Christine A.; Shah, Shivangi; Campion, Lindsey; Hakoum, Ahmad; Supnet, Melanie L.; Acuña, Patrick; Aldykiewicz, Gabrielle; Multhaupt‐Buell, Trisha; Ganza, Niecy G.M.; Lagarde, J. Benedict B.; Guzman, Jan Kristoper de; Go, Criscely L.; Currall, Benjamin; Trombetta, Bianca A.; Webb, Pia Kivisäkk; Talkowski, Michael E.; Arnold, Steven E.; Cheah, Pike See; Ito, Naoto; Sharma, Nutan; Bragg, D. Cristopher; Ozelius, Laurie J.; Breakefield, Xandra O.

doi:10.1002/mds.28305

Cited by 21 publications

(39 citation statements)

References 59 publications

(160 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…An extremely skewed (98%:2%) XCI was noted in only a single case with full XDP syndrome (Domingo et al, 2014), and X-chromosome monosomy (45,X/46,XX) was found in a subset of cells of another female patient with XDP(Westenberger et al, 2013). A recent study examining the peripheral blood of 17 carrier females (4 affected with parkinsonism and 13 non affected) (Al Ali et al, 2021), is also consistent with a mosaic XCI status being protective. Decreased full length TAF1 expression, as measured by the ratio of TAF1 3’/5’, is at an intermediate level for asymptomatic carriers such that XDP patients demonstrated the most reduction and asymptomatic female carriers demonstrated intermediate reduction compared to healthy controls.…”

Section: Discussionmentioning

confidence: 60%

“…Canonical TAF1 expression was decreased in various XDP samples, including fibroblast, RNA from blood and NSCs, compared to control samples (Al Ali et al, 2021; Aneichyk et al, 2018; Domingo et al, 2016; Ito et al, 2016). To quantify the 3’ region of canonical TAF1 expression in XDP female carrier-derived iPSCs, we performed RT-qPCR with primers targeting TAF1 exons 32 and 33 (Rakovic et al, 2018).…”

Section: Resultsmentioning

confidence: 89%

“…In contrast, female lines containing the active wild-type allele and silenced mutant allele had no detectable levels of TAF1-32i, a situation similar to control male iPSC lines and lines with a CRISPR-deleted SVA. A recent study demonstrated that TAF1-32i expression was elevated in XDP patients and female carriers compared to control samples but TAF1-32i expression levels did not distinguish carriers vs affected XDP patients (Al Ali et al, 2021). Our data suggest that the XDP haplotype is fully silenced by XCI and that TAF1-32i expression is a biomarker for XDP haplotype expression in female pluripotent stem cells.…”

Section: Discussionmentioning

confidence: 98%

“…XDP patient samples have decreased expression of the canonical full-length TAF1 ( cTAF1 ) transcript in dividing cells (Aneichyk et al, 2018; Rakovic et al, 2018), patient blood RNA (Al Ali et al, 2021), and a 2D cellular model of MSNs (Rakovic et al, 2018). The cTAF1 decreases are caused by the SVA, which induces alternative splicing and intron retention (Aneichyk et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Variation in TAF1 expression in female carrier induced pluripotent stem cells and human brain ontogeny has implications for adult neostriatum vulnerability in X-linked Dystonia Parkinsonism

D'Ignazio

Jacomini

Qamar

et al. 2022

Preprint

View full text Add to dashboard Cite

X-linked Dystonia-Parkinsonism (XDP) is an inherited, X-linked, adult-onset movement disorder characterized by degeneration in the neostriatum. No therapeutics alter disease progression. The mechanisms underlying regional differences in degeneration and age of onset are unknown. Developing therapeutics that target XDP-related mechanisms requires a deeper understanding of how XDP-relevant features vary in health and disease. XDP is due, in part, to either a partial loss of TAF1 function and/or a SVA-driven pathological gain of function. A disease-specific SINE-VNTR-Alu (SVA) retrotransposon insertion occurs within intron 32 of TAF1, a subunit of TFIID involved in transcription initiation. While all XDP males are usually clinically affected, females are heterozygous carriers generally not manifesting the full syndrome. As a resource for disease modeling, we characterized eight iPSC lines from XDP female carrier individuals, and identified isogenic lines where one clonal iPSC line expressed the wild-type X, and the two other clonal iPSC lines expressed the XDP haplotype. Furthermore, we characterized XDP-relevant transcript expression variation in humans, and found that SVA-F expression decreases slightly after 30 years of age in the neurotypical human brain and that TAF1 is modestly decreased in the majority of female samples. Uniquely in the caudate nucleus, TAF1 expression is not sexually dymorphic and decreased after 15 years of age. These findings indicate that regional-, age- and sex-specific mechanisms regulate TAF1, highlighting the importance of disease-relevant models and postmortem tissue analysis. We propose that the decreased TAF1 expression in the adult caudate may synergize with the XDP-specific partial loss of TAF1 function in patients, thereby passing a minimum threshold of TAF1 function, and triggering degeneration in the neostriatum.

show abstract

Section: Discussionmentioning

confidence: 60%

Section: Resultsmentioning

confidence: 89%

Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Variation in TAF1 expression in female carrier induced pluripotent stem cells and human brain ontogeny has implications for adult neostriatum vulnerability in X-linked Dystonia Parkinsonism

D'Ignazio

Jacomini

Qamar

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…Among the thirteen disease-specific variants is a ∼2.6 kb SINE-VNTR-Alu (SVA)-type retrotransposon [21] inserted in intron 32 of TAF1 [19]. XDP patient tissues and cell lines exhibit reduced TAF1 expression [19,20,22–25] as well as aberrant splicing that results in partial retention of intronic sequence proximal to the SVA insertion [20]. Reduced TAF1 expression, intron retention and aberrant splicing can be rescued by excision of the SVA [20,23], suggesting that SVA-mediated TAF1 transcriptional dysregulation may contribute to disease pathogenesis.…”

Section: Introductionmentioning

confidence: 99%

Tissue-specific and repeat length-dependent somatic instability of the X-linked dystonia parkinsonism-associated CCCTCT repeat

Campion

Yadav

Penney

et al. 2022

Preprint

Self Cite

View full text Add to dashboard Cite

X-linked dystonia-parkinsonism (XDP) is a progressive adult-onset neurodegenerative disorder caused by insertion of a SINE-VNTR-Alu (SVA) retrotransposon in the TAF1 gene. The SVA retrotransposon contains a CCCTCT hexameric repeat tract of variable length, whose length is inversely correlated with age at onset. This places XDP in a broader class of repeat expansion diseases, characterized by the instability of their causative repeat mutations. Here, we observe similar inverse correlations between CCCTCT repeat length with age at onset and age at death and no obvious correlation with disease duration. To gain insight into repeat instability in XDP we performed comprehensive quantitative analyses of somatic instability of the XDP CCCTCT repeat in blood and in seventeen brain regions from affected males. Our findings reveal repeat length-dependent and expansion-based instability of the XDP CCCTCT repeat, with greater levels of expansion in brain than in blood. The brain exhibits regional-specific patterns of instability that are broadly similar across individuals, with cerebellum exhibiting low instability and cortical regions exhibiting relatively high instability. The spectrum of somatic instability in the brain includes a high proportion of moderate repeat length changes of up to 5 repeats, as well as expansions of ~20->100 repeats and contractions of ~20-40 repeats at lower frequencies. Comparison with HTT CAG repeat instability in postmortem Huntington disease brains reveals similar brain region-specific profiles, indicating common trans-acting factors that contribute to the instability of both repeats. Analyses in XDP brains of expansion of a different SVA-associated CCCTCT located in the LIPG gene, and not known to be disease-associated, reveals repeat length-dependent expansion at overall lower levels relative to the XDP CCCTCT repeat, suggesting that expansion propensity may be modified by local chromatin structure. Together, the data support a role for repeat length-dependent somatic expansion in the process(es) driving the onset of XDP and prompt further investigation into repeat dynamics and the relationship to disease.

show abstract

X-linked dystonia parkinsonism: epidemiology, genetics, clinical features, diagnosis, and treatment

2022

View full text Add to dashboard Cite

TAF1 Transcripts and Neurofilament Light Chain as Biomarkers for X‐linked Dystonia‐Parkinsonism

Cited by 21 publications

References 59 publications

Variation in TAF1 expression in female carrier induced pluripotent stem cells and human brain ontogeny has implications for adult neostriatum vulnerability in X-linked Dystonia Parkinsonism

Variation in TAF1 expression in female carrier induced pluripotent stem cells and human brain ontogeny has implications for adult neostriatum vulnerability in X-linked Dystonia Parkinsonism

Tissue-specific and repeat length-dependent somatic instability of the X-linked dystonia parkinsonism-associated CCCTCT repeat

X-linked dystonia parkinsonism: epidemiology, genetics, clinical features, diagnosis, and treatment

Contact Info

Product

Resources

About