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. 2018 Nov 27;2018(11):CD012345. doi: 10.1002/14651858.CD012345.pub3

GLAMT 1993.

Methods Gamma Linolenic Acid Multicentre Trial (GLAMT)
RCT, 2‐arm, parallel (n6 GLA vs non‐fat), 1 year
Summary risk of bias: moderate to high
Participants People with mild diabetic neuropathy
 CVD risk: moderate
 Control: randomised 57, analysed 48 (with ≥ 1 evaluation)
 Intervention: randomised 54, analysed 52
 Mean years in trial: control 1.0, randomised 1.0
 % male: intervention 67%, control 79%,
 Age, mean (SD) years: intervention 53.3 (11.1), control 52.9 (11.4)
Age range: unclear
Smokers: unclear
Hypertension: unclear
Medications taken by ≥ 50% of those in the control group: insulin
Medications taken by 20%‐49% of those in the control group: not reported
Medications taken by some, but < 20% of the control group: not reported
Location: UK and Finland
Ethenicty: not reported
Interventions Type: supplement
Comparison: GLA (n‐6) vs placebo (paraffin)
Control aims: 12 capsules/d paraffin
 Intervention aims: 12 capsules/d evening primrose oil (EP4, equivalent to Epogam): 0.48 g/d GLA plus LA (stated as the major constituent, dose not given, if assume 0.7 g/capsule then 8.4 g/d*)
Dose aim: increase 0.48 g/d GLA or 4 kcal or 0.2% E GLA, increase ˜8.4 g/d LA or 76 kcal or 3.8% E LA, total 4% E n6
Baseline PUFA: unclear
Compliance by biomarkers: unclear, no serum TC or tissue fatty acid levels reported
Compliance by dietary intake: unclear

  • Energy intake: not reported

  • Total fat intake: not reported

  • SFA intake: not reported

  • PUFA intake: not reported

  • PUFA n‐3 intake: not reported

  • PUFA n‐6 intake: not reported

  • Trans fat intake: not reported

  • MUFA intake: not reported

  • CHO intake: not reported

  • Sugars intake: not reported

  • Protein intake: not reported

  • Alcohol intake: not reported


Compliance, other methods: not reported
Inclusion basis: aimed to increase GLA intake rather than total PUFA.
Dose aim appeared to be ˜4% E PUFA (from omega‐6 data), >10% more than assumed baseline of 6% E PUFA. No confirmatory biomarker or intake data
PUFA dose: 4% E PUFA (estimated from aim)
Duration of intervention: 1 year
Outcomes Main trial outcome: measures of diabetic neuropathy
 Dropouts: intervention 10, control 17
 Available outcomes: MI, cancer (no deaths)
Response to contact: contact attempted but no response to date.
Notes Trial funding: Scotia Pharmaceuticals
Risk of bias
Bias Authors' judgement Support for judgement
Random sequence generation (selection bias) Unclear risk Not described
Allocation concealment (selection bias) Unclear risk Not described
Blinding of participants and personnel (performance bias) 
 All outcomes Low risk Described as double‐blind, and
Quote: "Active and placebo capsules were indistinguishable in taste or appearance"
Blinding of outcome assessment (detection bias) 
 All outcomes Unclear risk Unclear, though trial described as double‐blind no methods or statement of blinding of outcome assessors was mentioned
Incomplete outcome data (attrition bias) 
 All outcomes High risk Reasons for withdrawal usually given, but high and dissimilar
Selective reporting (reporting bias) Unclear risk No clear protocol or trials registry entry found
Attention bias Low risk Appeared similar
Compliance Unclear risk Neither tissue PUFA biomarkers nor TC data reported
Other bias Low risk None identified