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| ID | Type | Description | Link |
|---|---|---|---|
| ACTRN12614000327684 | Registry Identifier | ANZCTR | |
| Project Grant GNT1057968 | Other Grant/Funding Number | NHMRC |
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Wernicke-Korsakoff syndrome (WKS), once thought to be a rare condition, is now known to be common in people with nutritional deficiencies or alcohol dependence. The primary cause of WKS is thiamine deficiency, and more than 90% of cases are reported in alcohol dependent patients because alcohol dependence predisposes to severe nutritional deficiency. WKS may lead to significant, long-term brain dysfunction with severe effects on work, personal and social function. Whilst effective treatment may greatly reduce severe disability and the human and social costs of this illness, almost no evidence exists on optimal dosing regimens. This project proposes to develop quality evidence for effective treatment of WKS in an Aboriginal setting.
Wernicke-Korsakoff syndrome (WKS), once thought to be a rare condition, is now known to be common in people with nutritional deficiencies or alcohol dependence. The primary cause of WKS is thiamine deficiency, and more than 90% of cases are reported in alcohol dependent patients because alcohol dependence predisposes to severe nutritional deficiency. WKS may lead to significant, long-term brain dysfunction with severe effects on work, personal and social function. Whilst effective treatment may greatly reduce severe disability and the human and social costs of this illness, almost no evidence exists on optimal dosing regimens. This project proposes to develop quality evidence for effective treatment of WKS in an Aboriginal setting..
The need for evidence-based thiamine treatment protocols is of great clinical importance for two related reasons. First, in relation to acute symptomatic WKS, a failure to treat immediately or adequately may result in profound and often permanent cognitive and neurological disability. Secondly, the need for evidence-based treatment guidelines is greatly magnified when it is recognised that milder, subclinical WKS may be preventable with adequate thiamine treatment.
The aims of this study are to determine the optimal thiamine dose required for:
A. Treatment of acute symptomatic WKS among Aboriginal and non-Aboriginal alcohol dependent patients.
B. Reducing or preventing subclinical WKS-related brain damage in at-risk Aboriginal and non-Aboriginal alcohol-dependent patients.
Primary Hypotheses
Secondary Hypotheses
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Acute Symptomatic WKS- 300mg | Active Comparator | Thiamine Hydrochloride 300mg daily (i.e. 100mg 3 times/day) for 5 days |
|
| Acute Symptomatic WKS - 900mg | Active Comparator | Thiamine Hydrochloride 900mg daily (i.e. 300mg 3 times/day) for 5 days |
|
| Acute Symptomatic WKS - 1500mg | Active Comparator | Thiamine Hydrochloride 1500mg daily (i.e. 500mg 3 times/day) for 5 days. |
|
| High-risk subclinical WKS- 100mg | Active Comparator | Thiamine Hydrochloride 100mg once daily for 3 days. |
|
| High-risk subclinical WKS- 300mg | Active Comparator | Thiamine Hydrochloride 300mg (i.e. 100mg 3 time/day) for 3 days |
|
| High-risk subclinical WKS - 900mg | Active Comparator |
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Thiamine Hydrochloride | Drug | Administered Intravenously in 100ml bag of normal saline (0.9%) infused over 30 mins. |
|
| Measure | Description | Time Frame |
|---|---|---|
| Standardised Cognitive assessment - RUDAS | Evaluate differences in cognitive outcomes among acute symptomatic WKS patients under three parenteral thiamine treatment conditions (300mg/day for 5 days, versus 900mg/day for 5 days, versus 1500mg/day for 5 days); and among patients at high risk of subclinical WKS-related brain damage under three parenteral thiamine treatment conditions (100mg/day for 3 days, versus 300mg/day for 3 days, versus 900mg/day for 3 days); using Standardised cognitive assessment - Rowland Universal Dementia Assessment Scale (RUDAS). | Days 1 and 5 for Acute symptomatic patients and Days 1 and 3 for at risk patients |
| Standardised Cognitive assessment - CogState | Evaluate differences in cognitive outcomes among acute symptomatic WKS patients under three parenteral thiamine treatment conditions (300mg/day for 5 days, versus 900mg/day for 5 days, versus 1500mg/day for 5 days); and among patients at high risk of subclinical WKS-related brain damage under three parenteral thiamine treatment conditions (100mg/day for 3 days, versus 300mg/day for 3 days, versus 900mg/day for 3 days); using CogState battery. | Days 1 and 5 for Acute symptomatic patients and Days 1 and 3 for at risk patients |
| Standardised Cognitive assessment - Story Memory Recall Test | Evaluate differences in cognitive outcomes among acute symptomatic WKS patients under three parenteral thiamine treatment conditions (300mg/day for 5 days, versus 900mg/day for 5 days, versus 1500mg/day for 5 days); and among patients at high risk of subclinical WKS-related brain damage under three parenteral thiamine treatment conditions (100mg/day for 3 days, versus 300mg/day for 3 days, versus 900mg/day for 3 days); using Story Memory Recall test | Days 1 and 5 for Acute symptomatic patients and Days 1 and 3 for at risk patients |
| Standardised neurological examination | Evaluate differences in neurological outcomes among acute symptomatic WKS patients under three parenteral thiamine treatment conditions (300mg/day for 5 days, versus 900mg/day for 5 days, versus 1500mg/day for 5 days);and among patients at high-risk of subclinical WKS-related brain damage under three parenteral thiamine treatment conditions (100mg/day for 3 days, versus 300mg/day for 3 days, versus 900mg/day for 3 days); Using Standardised neurological examination. Aggregated as either normal or abnormal. |
| Measure | Description | Time Frame |
|---|---|---|
| Blood thiamine levels | Correlate changes in red cell thiamine test results (blood test) with cognitive (standardised cognitive assessments score) and neurological functioning (standardised neurological examination). | Days 1 and 5 for acute symptomatic patients; days 1 and 3 for at risk patients |
| Magnesium levels |
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Inclusion Criteria:
Exclusion Criteria:
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| Name | Affiliation | Role |
|---|---|---|
| Kylie Dingwall, PhD | Menzies School of Health Research | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Alice Springs Hospital | Alice Springs | Northern Territory | 0810 | Australia |
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| ID | Term |
|---|---|
| D020915 | Korsakoff Syndrome |
| D009461 | Neurologic Manifestations |
| D000092862 | Psychological Well-Being |
| ID | Term |
|---|---|
| D008569 | Memory Disorders |
| D019954 | Neurobehavioral Manifestations |
| D009422 | Nervous System Diseases |
| D012816 | Signs and Symptoms |
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| ID | Term |
|---|---|
| C000712172 | thiamine hydrochloride |
| D013831 | Thiamine |
| D014803 | Vitamin B Complex |
| ID | Term |
|---|---|
| D013844 | Thiazoles |
| D013457 | Sulfur Compounds |
| D009930 | Organic Chemicals |
| D001393 | Azoles |
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Thiamine Hydrochloride 900mg daily (i.e. 300mg 3 times/day) for 3 days. |
|
|
| Days 1 and 5 for acute symptomatic patients; Days 1 and 3 for at risk patients |
Examine the impact of magnesium deficiency (magnesium blood test) on thiamine treatment response (cognition as measured by standardised cognitive assessments and thiamine pyrophosphate levels as measured by blood test). |
| Days 1 and 5 for acute symptomatic patients; Days 1 and 3 for at risk patients |
| Demographic factors | Assess independent predictors of WKS including nutritional factors, substance use history and demographic factors assessed by questionnaire items including Nutritional Risk Assessment and AUDIT-C. | Day 1 |
| Readmission | Examine the impact of patient re-admission on red cell thiamine pyrophosphate levels (blood test) and cognitive and neurological functioning (standardised cognitive and neurological assessments) | Day 1 |
| D013568 | Pathological Conditions, Signs and Symptoms |
| D010549 | Personal Satisfaction |
| D001519 | Behavior |
| D006573 |
| Heterocyclic Compounds, 1-Ring |
| D006571 | Heterocyclic Compounds |
| D011743 | Pyrimidines |
| D014815 | Vitamins |
| D018977 | Micronutrients |
| D045505 | Physiological Effects of Drugs |
| D020228 | Pharmacologic Actions |
| D020164 | Chemical Actions and Uses |