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Assay to Measure Huntington's Disease Progression and Response to Treatment


Technology Benefits

Monitors the severity and progression of Huntington’s disease.   Allows improved determination of stage of disease or prediction of onset of HD symptoms.   Provides assays for the development of new therapeutic compounds for the treatment of HD, including identification of patient populations that may be best suited for a particular drug or clinical trial.   Assay is sensitive to progression in HD and more related to the etiopathology of HD than current imaging measures.


Detailed Technology Description

Researchers at UCI have developed an assay to monitor the progression of Huntington's Disease utilizing a subjects' cerebrial spinal fluid (CSF).  It was discovered that CSF from HD patients, when put into contact with cells expressing expanded polyglutamine Httn variants, has the ability to increase aggregation of the Httn variants within the cells. This activity, referred to as "seeding", is measured by the number of cells with aggregates and by the amount of aggregates within the cells. This enhanced aggregation is quantifiable in HD CSF and used as a measure of disease presence, HD progression or remission, including the effects of various HD therapeutic interventions.  The below figure illustrates the assay.   Schematic of assay. Cells in tissue culture plate express mHttn, after adding CSF, aggregation is measured after 16 and 24 hrs   Future Development Plans Ongoing experiments will evaluate the correlation between enhanced aggregation in patients with pre-symptomatic and different stages of symptomatic HD to validate the assay.  We are interested in partnering with companies that wish to utilize this assay in their HD drug development programs or to further develop the assay for clinical use.


Application No.

20160178645


Others

Publications

http://www.ncbi.nlm.nih.gov/pubmed/26100538 Huntington's disease cerebrospinal fluid seeds aggregation of mutant huntingtin. Mol Psychiatry (2015) 1-8.

 


Tech ID/UC Case

23325/2013-804-0


Related Cases

2013-804-0


Country/Region

USA

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