Sporadic Degenerative Ataxia With Adult Onset: Natural History Study

Late Onset Sporadic Cerebellar Ataxia Clinical Trial

— SPORTAX-NHS  

Official title:

Sporadic Degenerative Ataxia With Adult Onset: Natural History Study (SPORTAX-NHS)

Clinical Trial Details — Status: Recruiting

Administrative data

• NCT number: NCT02701036
• Other study ID #: SPORTAX 010/05
• Status: Recruiting
• Phase: N/A
• First received: January 28, 2016
• Last updated: June 28, 2017
• Start date: April 2010
• Est. completion date: December 2030

Study information

• Verified date: June 2017
• Source: Ataxia Study Group
• Contact: Ilaria Anna Giordano, MD
• Phone: 0049 228 287 15750
• Email: ilaria_anna.giordano[@]ukb.uni-bonn.de
• Is FDA regulated: No
• Study type: Observational [Patient Registry]

Clinical Trial Summary

The key goals of SPORTAX-NHS is to compare the phenotype of multiple system atrophy of cerebellar type (MSA-C) and sporadic adult onset ataxia of unknown aetiology (SAOA) and to determine the rate of disease progression in both groups including determination of the factors that predict the development of MSA-C vs. SAOA, and at which time after onset of ataxia, a reliable distinction between both disorders is possible.

The planned study will also allow to collect blood samples and other biomaterials from patients with sporadic ataxia, which will be useful for future genetic and biomarker studies.

Description:

Progressive ataxia frequently starts in adults without a familial background. These patients may suffer from an acquired ataxia or a genetically determined ataxia despite negative family history. In the majority of them, however, a genetic or acquired cause of ataxia cannot be identified suggesting a sporadic degenerative ataxia. They can be subdivided into two groups. In one group, the underlying brain disease is multiple system atrophy (MSA), specifically MSA of cerebellar type (MSA-C). The characteristic clinical feature of MSA is the presence of severe autonomic failure defined by orthostatic hypotension or urinary incontinence. The second group is distinguished from MSA-C by the lasting absence of severe autonomic failure. These patients have been designated as sporadic adult onset ataxia of unknown aetiology (SAOA). In the first years after ataxia onset, a distinction between MSA-C and SAOA is often not possible.

There are only few studies comparing the phenotype of MSA-C and SAOA, and longitudinal studies focussing on the evolution of the phenotype of these disorders are completely lacking. In particular, the progression rate of SAOA compared to MSA-C has not been defined. In addition, it is unknown which factors predict the development of MSA-C vs. SAOA, and at which time after onset of ataxia, a reliable distinction between both disorders is possible.

To answer these questions, we plan to create a European registry of patients with sporadic degenerative ataxia of adult onset and to perform a natural history study. The planned study will also allow to collect blood samples and other biomaterials from patients with sporadic ataxia, which will be useful for future genetic and biomarker studies.

Recruitment information / eligibility

• Status: Recruiting
• Enrollment: 300
• Est. completion date: December 2030
• Est. primary completion date: December 2030
• Accepts healthy volunteers: Accepts Healthy Volunteers
• Gender: All
• Age group: 40 Years and older

Eligibility

Inclusion Criteria:

• Progressive ataxia

• Disease onset after the age of 40 years

• Informative and negative family history (no similar disorders in first- and second-degree relatives; parents older than 50 years, or, if not alive, age at death of more than 50 years, no consanguinity of parents)

Exclusion Criteria:

• No established acquired cause of ataxia

Clinical exclusion criteria:

• No onset of ataxia in association with stroke, encephalitis, sepsis, hyperthermia or heat stroke;

• no chronic diarrhea;

• no unexplained visual loss;

• no alcohol abuse;

• no chronic intake of anticonvulsant drugs;

• no other toxic causes; no malignancies;

• no rapid progression (development of severe ataxia in less than 12 weeks);

• no insulin-dependent diabetes mellitus

Imaging exclusion criteria:

• No evidence of multiple sclerosis, ischemia, hemorrhage or tumor of the posterior fossa;

• absence of signal abnormalities on T2/FLAIR-images except abnormalities compatible with MSA

Laboratory exclusion criteria:

• Negative molecular genetic testing for FRDA (only required if there is no cerebellar atrophy on MRI, SCA1, SCA2, SCA3, SCA6, FMR1 premutation (only required if prominent tremor, cognitive impairment and signal abnormality on T2/FLAIR images in the middle cerebellar peduncle);

• antineuronal antibodies negative (only required, if disease duration less than 3 years);

• normal levels of vitamin B12;

• VDRL negative;

• normal thyreoid function

Related Conditions & MeSH terms

• Ataxia
• Cerebellar Ataxia
• Late Onset Sporadic Cerebellar Ataxia

Locations

Country	Name	City	State
Austria	Department of Neurology, Medical University, Innsbruck	Innsbruck
Germany	Universitätsmedizin Berlin Charité	Berlin
Germany	Department of Neurology, University of Bonn	Bonn
Germany	Department of Neurology, University Clinic Essen, University of Duisburg-Essen	Essen
Germany	Department of Neurology, University of Frankfurt	Frankfurt
Germany	Hamburg UKE Abt. Neuropädiatrie	Hamburg
Germany	Otto-von-Guericke Universität Magdeburg	Magdeburg
Germany	Friedrich-Baur-Institut an der Neurologischen Klinik	München
Germany	Universitätsmedidzin Rostock - Klinik und Poliklinik für Neurologie	Rostock
Germany	Dept. of Neurodegenerative Diseases Tübingen	Tübingen
Italy	Department of Neuroscience, Federico II University Naples	Naples
Italy	Universita cattolica del sacro cuore	Rome
Netherlands	Radboud University Medical Center, Department of Neurology, Donders Institute for Brain, Cognition, and Behaviour	Nijmegen
Norway	Oslo University Hospital	Oslo

Sponsors (2)

Lead Sponsor	Collaborator
Ataxia Study Group	German Center for Neurodegenerative Diseases (DZNE)

Countries where clinical trial is conducted

Austria,  Germany,  Italy,  Netherlands,  Norway, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Scale for the assessment and rating of ataxia (SARA)	Both conditions (SAOA and MSAc) are part of neurodegenerative diseases, chronic progressive disorders. Their disease progression, can be measured using a validated ataxia scale, SARA. SARA was evaluated in two large validation trials performed by the EUROSCA clinical group and was found to be easy to use, reliable, and valid.	through study completion, an average of 10 years
Secondary	Inventory of non-ataxia signs (INAS)	The occurrence of accompanying non-ataxia symptoms is recorded using INAS.	through study completion, an average of 10 years
Secondary	spinocerebellar ataxia functional index (SCAFI)	to assess the severity of ataxia in an objective way, three quantitative tests, 8m-walk, 9HPT (hole peg test) and PATA rate (timed speech task) are used.	through study completion, an average of 10 years
Secondary	Unified Multiple System Atrophy Rating Scale (UMSARS)	UMSARS is a validated scale for multiple system atrophy used to assess additional symptoms typically occurring in MSA. The scale comprises the following components: Part I, historical, 12 items; Part II, motor examination, 14 items; Part III, autonomic examination; and Part IV, global disability scale.	through study completion, an average of 10 years
Secondary	Questionnaire for Cerebellar Multisystem Atrophy diagnostic criteria	To distinguish between SAOA and MSAc adjusted criteria for multiple system atrophy of cerebellar type on the basis of consensus statement on the diagnostic criteria for MSAc are used (Second consensus statement on the diagnosis of multiple system atrophy: Neurology. 2008 Aug 26; 71(9): 670-676).; Probable MSAc requires a sporadic, progressive adult-onset disorder including rigorously defined autonomic failure and cerebellar ataxia. Possible cerebellar MSA requires a sporadic, progressive adult-onset disease including cerebellar ataxia and at least one feature suggesting autonomic dysfunction plus one other feature that may be a clinical or a neuroimaging abnormality (Babinski sign with hyperreflexia, Stridor, Parkinsonism (bradykinesia and rigidity), Atrophy on MRI of putamen, middle cerebellar peduncle, or pons, Hypometabolism on FDG-PET in putamen, Presynaptic nigrostriatal dopaminergic denervation on SPECT or PET. If both criteria are not met patient is classified as a SAOA.	through study completion, an average of 10 years
Secondary	EQ-5D	Health related Quality of life is assessed using EQ-5D, a generic instrument that has been developed and validated by the EuroQuol Group (1990) and is available in validated translations for use as a questionnaire.	through study completion, an average of 10 years
Secondary	PHQ-9	Assessment of depressive symptoms is done using a validated 9-item short form of the Patient Health Questionnaire (PHQ), a questionnaire that has been developed to screen for psychiatric co-morbidity in unselected populations	through study completion, an average of 10 years
Secondary	Comparison of phenotype of cerebellar multiple system atrophy and sporadic adult onset ataxia of unknown etiology	classified as "SAOA" can convert into MSAc, that is why they are followed with yearly clinical assessments.	through study completion, an average of 10 years
Secondary	RBDSQ	REM Behaviour Disorder Screening Questionnaire (RBDSQ)	through study completion, an average of 10 years

External Links

•   Sportax Database