Meso scale discovery-based assays for the detection of aggregated huntingtin

Wolfgang Reindl; Barbara Baldo; Jana Schulz; Isabell Janack; Ilka Lindner; Markus Kleinschmidt; Yalda Sedaghat; Christina Thiede; Karsten Tillack; Christina Schmidt; Isabell Cardaun; Tom Schwagarus; Frank Herrmann; Madlen Hotze; Georgina F Osborne; Simone Herrmann; Andreas Weiss; Celina Zerbinatti; Gillian P Bates; Jonathan Bard; Ignacio Munoz-Sanjuan; Douglas Macdonald

doi:10.1371/journal.pone.0213521

Meso scale discovery-based assays for the detection of aggregated huntingtin

PLoS One. 2019 Mar 26;14(3):e0213521. doi: 10.1371/journal.pone.0213521. eCollection 2019.

Authors

Wolfgang Reindl¹, Barbara Baldo¹, Jana Schulz¹, Isabell Janack¹, Ilka Lindner¹, Markus Kleinschmidt¹, Yalda Sedaghat¹, Christina Thiede¹, Karsten Tillack¹, Christina Schmidt¹, Isabell Cardaun¹, Tom Schwagarus¹, Frank Herrmann¹, Madlen Hotze¹, Georgina F Osborne², Simone Herrmann¹, Andreas Weiss¹, Celina Zerbinatti¹, Gillian P Bates², Jonathan Bard³, Ignacio Munoz-Sanjuan³, Douglas Macdonald³

Affiliations

¹ Evotec AG, Hamburg, Germany.
² Dept. Neurodegenerative Disease, Huntington's Disease Centre and Dementia Research Institute, Institute of Neurology, University College London, London, United Kingdom.
³ CHDI Management/CHDI Foundation, Los Angeles, CA, United States of America.

Abstract

Huntington's disease (HD) is a monogenic neurodegenerative disorder caused by an expansion of the CAG trinucleotide repeat domain in the huntingtin (HTT) gene, leading to an expanded poly-glutamine (polyQ) stretch in the HTT protein. This mutant HTT (mHTT) protein is highly prone to intracellular aggregation, causing significant damage and cellular loss in the striatal, cortical, and other regions of the brain. Therefore, modulation of mHTT levels in these brain regions in order to reduce intracellular mHTT and aggregate levels represents a direct approach in the development of HD therapeutics. To this end, assays that can be used to detect changes in HTT levels in biological samples are invaluable tools to assess target engagement and guide dose selection in clinical trials. The Meso Scale Discovery (MSD) ELISA-based assay platform is a robust and sensitive method previously employed for the quantification of HTT. However, the currently available MSD assays for HTT are primarily detecting the monomeric soluble form of the protein, but not aggregated species. In this study, we describe the development of novel MSD assays preferentially detecting mHTT in an aggregated form. Recombinant monomeric HTT(1-97)-Q46, which forms aggregates in a time-dependent manner, was used to characterize the ability of each established assay to distinguish between HTT monomers and HTT in a higher assembly state. Further validation of these assays was performed using brain lysates from R6/2, zQ175 knock-in, and BACHD mouse models, to replicate a previously well-characterized age-dependent increase in brain aggregate signals, as well as a significant reduction of aggregate levels in the striatum following mHTT knockdown with a CAG-directed allele-specific zinc-finger repressor protein (ZFP). Lastly, size exclusion chromatography was used to separate and characterize HTT species from brain tissue lysates to demonstrate specificity of the assays for the fractions containing aggregated HTT. In summary, we demonstrate that the newly developed assays preferentially detect aggregated HTT with improved performance in comparison to previous assay technologies. These assays complement the existing MSD platform assays specific for soluble HTT monomers, allowing for a more comprehensive analysis of disease-relevant HTT species in preclinical models of HD.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Biological Assay*
Brain / metabolism*
Disease Models, Animal
Humans
Huntingtin Protein / genetics
Huntingtin Protein / metabolism*
Huntington Disease / genetics
Huntington Disease / metabolism*
Huntington Disease / pathology
Mice
Mice, Transgenic
Peptides / genetics
Peptides / metabolism*
Protein Aggregation, Pathological / genetics
Protein Aggregation, Pathological / metabolism*
Protein Aggregation, Pathological / pathology

Substances

HTT protein, human
Huntingtin Protein
Peptides
polyglutamine

Grants and funding

CHDI Foundation is a privately-funded not-for-profit biomedical research organization exclusively dedicated to discovering and developing therapeutics that slow the progression of Huntington’s Disease. CHDI Foundation conducts research in a number of different ways; for the purposes of this manuscript, research was conducted at the contract research organization Evotec AG under fee-for-service agreements. The listed authors all contributed to the conception, planning, and direction of the research, including generation, analysis, and interpretation of the data.