The effects of probucol on the progression of atherosclerosis in mature Watanabe heritable hyperlipidaemic rabbits

1 Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham‐treated diet at 9 months and followed for 6 months (n = 8); Group...

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Published inBritish journal of pharmacology Vol. 103; no. 1; pp. 1013 - 1018
Main Authors Daugherty, Alan, Zweifel, Ben S., Schonfeld, Gustav
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.05.1991
Nature Publishing
Subjects
Animals
Arteriosclerosis - drug therapy
Arteriosclerosis - genetics
Arteriosclerosis - pathology
atherosclerosis
Biological and medical sciences
cholesterol
Cholesterol - blood
General and cellular metabolism. Vitamins
Hyperlipidemias - complications
Hyperlipidemias - genetics
Lipids - blood
Lipoproteins, LDL - blood
Medical sciences
oxidation
Oxidation-Reduction
Pharmacology. Drug treatments
Probucol
Probucol - blood
Probucol - therapeutic use
Rabbits
Watanabe heritable hyperlipidaemic rabbits
Rabbit
Cardiovascular disease
Lipids
Metabolic diseases
Lagomorpha
Cholesterol
Vascular disease
Vertebrata
Chemotherapy
Mammalia
Treatment
Animal
Atherosclerosis
Hyperlipemia
Antilipemic agent
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Abstract 1 Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham‐treated diet at 9 months and followed for 6 months (n = 8); Group III placed on probucol at 9 months and followed for 6 months (n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. 2 Plasma concentrations of probucol increased to 93 ± 11 μg ml−1 in Group III during the initial 2 weeks and increased further to 149 ± 24 μg ml−1 at the end of the treatment period. 3 Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. 4 No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol‐treated rabbits. However, LDL from probucol‐treated animals was resistant to oxidation in the presence of Cu2+ (3 μm). 5 Group I had aortic atherosclerosis covering 70 ± 5% of intimal area of thoracic aortae, that increased to 91 ± 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 ± 0.2 μg mg−1 in Group I to 2.7 ± 0.3 μg mg−1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 ± 7%). However, probucol treatment reduced cholesterol content to 1.9 ± 0.3 μg mg−1 (P < 0.01). Collagen content of aortae was not affected by probucol treatment. 6 Thus, while probucol did not promote regression, the drug did retard the continued deposition of cholesterol esters into atherosclerotic lesions of mature WHHL rabbits.
AbstractList 1. Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (approximately 9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham-treated diet at 9 months and followed for 6 months (n = 8); Group III placed on probucol at 9 months and followed for 6 months (n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. 2. Plasma concentrations of probucol increased to 93 +/- 11 micrograms ml-1 in Group III during the initial 2 weeks and increased further to 149 +/- 24 micrograms ml-1 at the end of the treatment period. 3. Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. 4. No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol-treated rabbits. However, LDL from probucol-treated animals was resistant to oxidation in the presence of Cu2+ (3 microM). 5. Group I had aortic atherosclerosis covering 70 +/- 5% of intimal area of thoracic aortae, that increased to 91 +/- 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 +/- 0.2 microgram mg-1 in Group I to 2.7 +/- 0.3 microgram mg-1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 +/- 7%). However, probucol treatment reduced cholesterol content to 1.9 + 0.3,ugmg-' (P < 0.01). Collagen content of aortae was not affected by probucol treatment. 6. Thus, while probucol did not promote regression, the drug did retard the continued deposition of cholesterol esters into atherosclerotic lesions of mature WHHL rabbits.
1. Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (approximately 9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham-treated diet at 9 months and followed for 6 months (n = 8); Group III placed on probucol at 9 months and followed for 6 months (n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. 2. Plasma concentrations of probucol increased to 93 +/- 11 micrograms ml-1 in Group III during the initial 2 weeks and increased further to 149 +/- 24 micrograms ml-1 at the end of the treatment period. 3. Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. 4. No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol-treated rabbits. However, LDL from probucol-treated animals was resistant to oxidation in the presence of Cu2+ (3 microM). 5. Group I had aortic atherosclerosis covering 70 +/- 5% of intimal area of thoracic aortae, that increased to 91 +/- 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 +/- 0.2 microgram mg-1 in Group I to 2.7 +/- 0.3 microgram mg-1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 +/- 7%).
Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months ( n = 9); Group II placed on sham‐treated diet at 9 months and followed for 6 months ( n = 8); Group III placed on probucol at 9 months and followed for 6 months ( n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. Plasma concentrations of probucol increased to 93 ± 11 μg ml −1 in Group III during the initial 2 weeks and increased further to 149 ± 24 μg ml −1 at the end of the treatment period. Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol‐treated rabbits. However, LDL from probucol‐treated animals was resistant to oxidation in the presence of Cu 2+ (3 μ m ). Group I had aortic atherosclerosis covering 70 ± 5% of intimal area of thoracic aortae, that increased to 91 ± 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 ± 0.2 μg mg −1 in Group I to 2.7 ± 0.3 μg mg −1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 ± 7%). However, probucol treatment reduced cholesterol content to 1.9 ± 0.3 μg mg −1 ( P < 0.01). Collagen content of aortae was not affected by probucol treatment. Thus, while probucol did not promote regression, the drug did retard the continued deposition of cholesterol esters into atherosclerotic lesions of mature WHHL rabbits.
1. Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (approximately 9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham-treated diet at 9 months and followed for 6 months (n = 8); Group III placed on probucol at 9 months and followed for 6 months (n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. 2. Plasma concentrations of probucol increased to 93 +/- 11 micrograms ml-1 in Group III during the initial 2 weeks and increased further to 149 +/- 24 micrograms ml-1 at the end of the treatment period. 3. Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. 4. No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol-treated rabbits. However, LDL from probucol-treated animals was resistant to oxidation in the presence of Cu2+ (3 microM). 5. Group I had aortic atherosclerosis covering 70 +/- 5% of intimal area of thoracic aortae, that increased to 91 +/- 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 +/- 0.2 microgram mg-1 in Group I to 2.7 +/- 0.3 microgram mg-1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 +/- 7%). However, probucol treatment reduced cholesterol content to 1.9 + 0.3,ugmg-' (P &lt; 0.01). Collagen content of aortae was not affected by probucol treatment. 6. Thus, while probucol did not promote regression, the drug did retard the continued deposition of cholesterol esters into atherosclerotic lesions of mature WHHL rabbits.
1 Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and treated as follows: Group 1 killed at 9 months (n = 9); Group II placed on sham‐treated diet at 9 months and followed for 6 months (n = 8); Group III placed on probucol at 9 months and followed for 6 months (n = 8). Probucol was administered by mixing 1% wt/wt drug with standard laboratory diet. 2 Plasma concentrations of probucol increased to 93 ± 11 μg ml−1 in Group III during the initial 2 weeks and increased further to 149 ± 24 μg ml−1 at the end of the treatment period. 3 Plasma concentrations of total cholesterol, unesterified cholesterol and phospholipids were significantly reduced overall by probucol, while triglycerides were not affected. 4 No statistically significant differences were observed in the presence of oxidized products in low density lipoproteins (LDL) isolated from plasma of controls compared to probucol‐treated rabbits. However, LDL from probucol‐treated animals was resistant to oxidation in the presence of Cu2+ (3 μm). 5 Group I had aortic atherosclerosis covering 70 ± 5% of intimal area of thoracic aortae, that increased to 91 ± 3% in Group II. This was associated with cholesterol contents of aortae increasing from 1.4 ± 0.2 μg mg−1 in Group I to 2.7 ± 0.3 μg mg−1 in Group II. Probucol administration did not produce a statistically significant reduction of atherosclerotic lesion area (78 ± 7%). However, probucol treatment reduced cholesterol content to 1.9 ± 0.3 μg mg−1 (P < 0.01). Collagen content of aortae was not affected by probucol treatment. 6 Thus, while probucol did not promote regression, the drug did retard the continued deposition of cholesterol esters into atherosclerotic lesions of mature WHHL rabbits.
Author Daugherty, Alan
Zweifel, Ben S.
Schonfeld, Gustav
AuthorAffiliation Cardiovascular Division, Washington University School of Medicine, St. Louis, MO 63110
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Issue 1
Keywords Rabbit
Cardiovascular disease
Lipids
Metabolic diseases
Lagomorpha
Cholesterol
Vascular disease
Vertebrata
Chemotherapy
Mammalia
Treatment
Animal
Atherosclerosis
Hyperlipemia
Antilipemic agent
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SCHAFFNER T. (e_1_2_1_31_1) 1980; 100
e_1_2_1_10_1
e_1_2_1_33_1
e_1_2_1_2_1
e_1_2_1_32_1
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e_1_2_1_15_1
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e_1_2_1_9_1
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NARUSZEWICZ M. (e_1_2_1_22_1) 1984; 25
e_1_2_1_19_1
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Snippet 1 Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and...
1. Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (approximately 9 months old). Groups of WHHL rabbits were randomly...
Probucol was administered to mature Watanabe heritable hyperlipidaemic (WHHL) rabbits (≅9 months old). Groups of WHHL rabbits were randomly selected and...
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crossref
pubmed
pascalfrancis
wiley
SourceType Open Access Repository
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Index Database
Publisher
StartPage 1013
SubjectTerms Animals
Arteriosclerosis - drug therapy
Arteriosclerosis - genetics
Arteriosclerosis - pathology
atherosclerosis
Biological and medical sciences
cholesterol
Cholesterol - blood
General and cellular metabolism. Vitamins
Hyperlipidemias - complications
Hyperlipidemias - genetics
Lipids - blood
Lipoproteins, LDL - blood
Medical sciences
oxidation
Oxidation-Reduction
Pharmacology. Drug treatments
Probucol
Probucol - blood
Probucol - therapeutic use
Rabbits
Watanabe heritable hyperlipidaemic rabbits
Title The effects of probucol on the progression of atherosclerosis in mature Watanabe heritable hyperlipidaemic rabbits
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fj.1476-5381.1991.tb12293.x
https://www.ncbi.nlm.nih.gov/pubmed/1878742
https://search.proquest.com/docview/72056126
https://pubmed.ncbi.nlm.nih.gov/PMC1908069
Volume 103
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