Clinical Trials Logo
  1. Home
  2. Cognitive Impairment
  3. NCT03578796
  4. Details
NCT03578796 Clinical Trial

Edinburgh Cognitive and Behavioural Amyotrophic Lateral Sclerosis Screen in Norway: A Prospective Cohort Study

Cognitive Impairment Clinical Trial

Official title:
Cognitive Impairment in ALS: Screening Tools, Experiences and Prognosis

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT03578796
Other study ID # 2016/2187-1
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date May 1, 2017
Est. completion date December 31, 2022

Study information
Verified date March 2022
Source Haukeland University Hospital
Contact Tina Taule, PhD
Phone +47 41694143
Email tina.taule@helse-bergen.no
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

This study evaluate use of a translated Norwegian version of the Edinburgh cognitive and behavioral amyotrophic lateral sclerosis screen (ECAS-N) as an early predictor in car-driving, working and use of advanced life-prolonging therapy.

Description:

Cognitive impairment is present in about 30-50% of the patients with amyotrophic lateral sclerosis (ALS). Screening of cognitive and behavioral impairment is a distinct recommendation in ALS-specific health care. However, knowledge in how cognitive impairment shall influence health-care professionals' information given to patients and in decision making is lacking. One of the major challenges in ALS management is the decision-making on advanced therapy. There is a lack of knowledge in how cognitive impairment in ALS shall be interfere on complex medical treatment that will affect quality of life or life itself. This means significant implications not only to the ALS patient and the community, but also the family and especially the spouse. Thus, further investigation of the ECAS-N and its potential in clinical use is needed. The scale may contribute a more proactive treatment better tailored to individual needs. The objective is to evaluate if the ECAS-N can be applied as an early predictor in car-driving, working and use of advanced life-prolonging therapy

Recruitment information / eligibility
Status Recruiting
Enrollment 50
Est. completion date December 31, 2022
Est. primary completion date December 31, 2022
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - Voluntary informed consent - Native Norwegian speaker Exclusion Criteria: - Great difficulties in writing or reading - Comorbid medical history - Neurological disorders others than ALS - Psychiatric history of importance to cognitive function

Study Design

Related Conditions & MeSH terms

Intervention

Diagnostic Test:
ECAS-N
assessing ALS-specific cognitive impairment
MoCA
assessing cognitive impairment
CDR
assessing global cognitive impairment, as well as possible diagnosis- and Level of dementia
Other:
Questionnaire
Questions related to work situation and car driving

Locations
Country Name City State
Norway Haukeland University Hospital Bergen

Sponsors (2)
Lead Sponsor Collaborator
Haukeland University Hospital Western Norway University of Applied Sciences

Country where clinical trial is conducted

Norway, 

Outcome
Type Measure Description Time frame Safety issue
Other Edinburgh cognitive and behavioral amyotrophic lateral sclerosis screen-Norwegian Version (ECAS-N) We will use the ALS-specific sub-score (minimum score = 0, maximum score = 100), the ALS non-specific sub-score (minimum score = 0, maximum score = 36), a summed total ECAS-N score (minimum score =0, maximum score =136), the sub score of behavioural changes (minimum score = 0, maximum score = 10) and the sub score of psychotic change (minimum score = 0, maximum score = 3). A dichotomized cut-off scores for normality will also be used for the ALS-specific cut-off score of 65 or over, the non ALS-specific cut-off score of 24 or over and the total ECAS-N cut-off score of 92 or over. For the ALS-specific scores, non ALS-specific scores and total ECAS-N scores, high scores indicate less problems than low scores. For the sub score of behavioural change and the sub score of psychotic change, high scores indicate more problems than low scores. 4 months
Other Change from 4 months Edinburgh cognitive and behavioral amyotrophic lateral sclerosis screen-Norwegian Version (ECAS-N) at 8 months We will use the changed ALS-specific sub-score (minimum score = 0, maximum score = 100), the changed ALS non-specific sub-score (minimum score = 0, maximum score = 36), a changed summed total ECAS-N score (minimum score =0, maximum score =136), the changed sub score of behavioural changes (minimum score = 0, maximum score = 10) and the changed sub score of psychotic change (minimum score = 0, maximum score = 3). A changed dichotomized cut-off scores for normality will also be used for the ALS-specific cut-off score of 65 or over, the non ALS-specific cut-off score of 24 or over and the total ECAS-N cut-off score of 92 or over. For the ALS-specific scores, non ALS-specific scores and total ECAS-N scores, high scores indicate less problems than low scores. For the sub score of behavioural change and the sub score of psychotic change, high scores indicate more problems than low scores. 8 months
Other Montreal Cognitive Assessment (MoCA) We will use the total MoCA score (minimum score = 0, maximum score = 30) and a dichotomized cut-off score for normality of 26 or over. High scores indicate less problems than low scores 4 months
Other Change from 4 months Montreal Cognitive Assessment (MoCA) at 8 months We will use the changed total MoCA score (minimum score = 0, maximum score = 30) and the changed dichotomized cut-off score for normality of 26 or over. High scores indicate less problems than low scores 8 months
Primary Clinical Dementia Rating (CDR) We will use the total CDR score (minimum score = 0, maximum score = 18). Low scores indicate less problems than high scores. 8 months
Secondary Clinical Dementia Rating (CDR) We will use the total CDR score (minimum score = 0, maximum score = 18). Low scores indicate less problems than high scores. 4 months
Secondary Clinical Dementia Rating (CDR) We will use the total CDR score (minimum score = 0, maximum score = 18). Low scores indicate less problems than high scores. 3 years or until death
Secondary Ability in car-driving We will use a categorical variable (yes or no) and time of change to reduced function. 8 months
Secondary Ability in car-driving We will use a categorical variable (yes or no) and time of change to reduced function. 4 months
Secondary Ability in car-driving We will use a categorical variable (yes or no) and time of change to reduced function. 3 years or until death
Secondary Working ability We will use a categorical variable (yes or no) and time of change to reduced function. 8 months
Secondary Working ability We will use a categorical variable (yes or no) and time of change to reduced function. 4 months
Secondary Working ability We will use a categorical variable (yes or no) and time of change to reduced function. 3 years or until death
Secondary Use of Advanced life-prolonging therapy We will use a categorical variable (yes or no) and time of change to reduced function. 8 months
Secondary Use of Advanced life-prolonging therapy We will use a categorical variable (yes or no) and time of change to reduced function. 4 months
Secondary Use of Advanced life-prolonging therapy We will use a categorical variable (yes or no) and time of change to reduced function. 3 years or until death
See also
  Status Clinical Trial Phase
Completed NCT02122198 - Vascular Mechanisms for the Effects of Loss of Ovarian Hormone Function on Cognition in Women N/A
Recruiting NCT04356924 - Psychological Treatment to Support the Consequences of Cognitive Impairment N/A
Suspended NCT05542238 - The Effect of Acute Exercise on Cardiac Autonomic, Cerebrovascular, and Cognitive Function in Spinal Cord Injury N/A
Terminated NCT04493957 - Evaluation of an Educational Program in the Prevention of the Driving Risks in Patients With Neurocognitive Disorders : ACCOMPAGNE N/A
Recruiting NCT04792983 - Cognition and the Immunology of Postoperative Outcomes
Completed NCT06029920 - Influence of Overground Walking on Biomarkers, Cognitive Function, and Quality of Life in Elderly With Mild Cognitive Impairment N/A
Not yet recruiting NCT05068323 - Impact of Interictal Epileptiform Activity on Some Cognitive Domains in Newly Diagnosed Epileptic Patients N/A
Completed NCT04426838 - Cognitive Behavioral Therapy for Insomnia for the Dementia Caregiving Dyad N/A
Completed NCT04713384 - Remote Bimanual Virtual Rehabilitation Post CVD N/A
Recruiting NCT06284213 - Biomarkers for Vascular Contributions to Cognitive Impairment and Dementia Consortium
Recruiting NCT06053775 - Non-Invasive Brain Stimulation and Cognitive Training for Depressive Symptomatology Related to Breast Cancer (ONCODEP) N/A
Completed NCT03698695 - A Pharmacodynamics, Safety, and Pharmacokinetics Study of THN201 Versus Donepezil in Healthy Male Volunteers Phase 1
Not yet recruiting NCT05552729 - Effects of Different Doses of Vitamin D on Cancer-related Cognitive Impairment in Patients With Gastrointestinal Tumors Phase 1/Phase 2
Recruiting NCT03268109 - COGnitive ImpairmenT in Older HIV-infected Patients ≥ 65 Years Old
Completed NCT03187353 - IMProving Executive Function Study Phase 4
Completed NCT03301402 - Air Purifier to Improve Endothelial Function and Carotid Intima Thickness N/A
Completed NCT05395559 - Prevalence and Recognition of Cognitive Impairment in Hospitalized Patients: a Flash Mob Study
Recruiting NCT05030285 - Telehealth Psychotherapy for Anxiety in Persons With Cognitive Impairment N/A
Recruiting NCT04907565 - Impact of Obesity on Post-operative Cognitive Dysfunction: Role of Adipose Tissue
Recruiting NCT04897334 - Transcranial Direct Current Stimulation and Rehabilitation to Ameliorate Impairments in Neurocognition After Stroke N/A