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

Laura D'Ignazio; Ricardo S Jacomini; Bareera Qamar; Kynon J M Benjamin; Ria Arora; Tomoyo Sawada; Taylor A Evans; Kenneth E Diffenderfer; Aimee R Pankonin; William T Hendriks; Thomas M Hyde; Joel E Kleinman; Daniel R Weinberger; D Cristopher Bragg; Apua C M Paquola; Jennifer A Erwin

doi:10.1523/ENEURO.0129-22.2022

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

eNeuro. 2022 Jul 21;9(4):ENEURO.0129-22.2022. doi: 10.1523/ENEURO.0129-22.2022. Online ahead of print.

Authors

Laura D'Ignazio^{1

2}, Ricardo S Jacomini^{1

2}, Bareera Qamar¹, Kynon J M Benjamin^{1

2

3}, Ria Arora^{1

4}, Tomoyo Sawada^{1

2}, Taylor A Evans^{1

2}, Kenneth E Diffenderfer⁵, Aimee R Pankonin⁵, William T Hendriks^{6

7}, Thomas M Hyde^{1

3}, Joel E Kleinman^{1

3}, Daniel R Weinberger^{1

2

3

8

9}, D Cristopher Bragg^{6

7}, Apua C M Paquola^{1

2}, Jennifer A Erwin^{10

2

3

8}

Affiliations

¹ Lieber Institute for Brain Development, Baltimore, MD 21205, USA.
² Department of Neurology, School of Medicine, Johns Hopkins University, Baltimore, MD 21205, USA.
³ Department of Psychiatry & Behavioral Sciences, School of Medicine, Johns Hopkins University, Baltimore, MD 21205, USA.
⁴ Department of Biology, Krieger School of Arts & Sciences, Johns Hopkins University, Baltimore, MD 21218, USA.
⁵ Stem Cell Core, Salk Institute for Biological Studies, La Jolla, CA 92037, USA.
⁶ Department of Neurology, Massachusetts General Hospital and Harvard Medical School, Boston, MA 02114, USA.
⁷ The Collaborative Center for X-linked Dystonia-Parkinsonism, Massachusetts General Hospital, Charlestown, MA 02129, USA.
⁸ Department of Neuroscience, School of Medicine, Johns Hopkins University, Baltimore, MD 21205, USA.
⁹ McKusick-Nathans Department of Genetic Medicine, School of Medicine, Johns Hopkins University Baltimore, MD 21205, USA.
¹⁰ Lieber Institute for Brain Development, Baltimore, MD 21205, USA jennifer.erwin@libd.org.

Abstract

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 adult onset are unknown. Developing therapeutics requires a deeper understanding of how XDP-relevant features vary in health and disease. XDP is possibly due, in part, to a partial loss of TAF1 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 three XDP female carrier individuals for X chromosome inactivation status and identified clonal lines that express either the wild-type X or XDP haplotype. Furthermore, we characterized XDP-relevant transcript expression in neurotypical humans, and found that SVA-F expression decreases after 30 years of age in the brain and that TAF1 is decreased in most female samples. Uniquely in the caudate nucleus, TAF1 expression is not sexually dimorphic and decreased after adolescence. These findings indicate that regional-, age- and sex-specific mechanisms regulate TAF1, highlighting the importance of disease-relevant models and postmortem tissue. 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.Significance StatementXDP is an inherited, X-linked, adult-onset movement disorder characterized by degeneration in the neostriatum. No therapeutics alter disease progression. Developing therapeutics requires a deeper understanding of how XDP-relevant features vary in health and disease. XDP is possibly due to a partial loss of TAF1 function. While all XDP males are usually affected, females are heterozygous carriers generally not manifesting the full syndrome. As a resource for disease modeling, we characterized eight stem cell lines from XDP female carrier individuals. Furthermore, we found that, uniquely in the caudate nucleus, TAF1 expression decreases after adolescence in healthy humans. We hypothesize that the decrease of TAF1 after adolescence in human caudate, in general, may underlie the vulnerability of the adult neostriatum in XDP.

Keywords: SVA retrotransposon; X-linked Dystonia Parkinsonism; induced pluripotent stem cells; movement disorder; neurodegeneration; repeat expansion.

Grants and funding

T32 MH015330/MH/NIMH NIH HHS/United States