Pravastatin Reduces Marfan Aortic Dilation

Alexander Black

doi:10.1161/CIRCULATIONAHA.110.012187

Pravastatin Reduces Marfan Aortic Dilation

Alexander Black

Anatomy

Research output: Chapter in Book or Conference Publication/Proceeding › Conference Publication › peer-review

Abstract

Background-The sequelae of aortic root dilation are the lethal consequences of Marfan syndrome. The root dilation is attributable to an imbalance between deposition of matrix elements and metalloproteinases in the aortic medial layer as a result of excessive transforming growth factor-beta signaling. This study examined the efficacy and mechanism of statins in attenuating aortic root dilation in Marfan syndrome and compared effects to the other main proposed preventative agent, losartan.Methods and Results-Marfan mice heterozygous for a mutant allele encoding a cysteine substitution in fibrillin-1 (C1039G) were treated daily from 6 weeks old with pravastatin 0.5g L or losartan 0.6 g L. The end points of aortic root diameter (n = 25), aortic thickness, and architecture (n = 10), elastin volume (n = 5), dp dtmax (maximal rate of change of pressure) (cardiac catheter; n = 20), and ultrastructural analysis with stereology (electron microscopy; n = 5) were examined. The aortic root diameters of untreated Marfan mice were significantly increased in comparison to normal mice (0.161 + - 0.001 cm vs 0.252 + - 0.004 cm; P 0.01). Pravastatin (0.22 + - 0.003 cm; P 0.01) and losartan (0.221 + - 0.004 cm; P 0.01) produced a significant reduction in aortic root dilation. Both drugs also preserved elastin volume within the medial layer (pravastatin 0.23 + - 0.02 and losartan 0.29 + - 0.03 vs untreated Marfan 0.19 + - 0.02; P = 0.01; normal mice 0.27 + - 0.02). Ultrastructural analysis showed a reduction of rough endoplasmic reticulum in smooth muscle cells with pravastatin (0.022 + - 0.004) and losartan (0.013 + - 0.001) compared to untreated Marfan mice (0.035 + - 0.004; P 0.01).Conclusions-Statins are similar to losartan in attenuating aortic root dilation in a mouse model of Marfan syndrome. They appear to act through reducing the excessive protein manufacture by vascular smooth muscle cells, which occurs in the Marfan aorta. As a drug that is relatively well-tolerated for long-term use, it may be useful clinically. (Circulation. 2011; 124[suppl 1]: S168-S173.)

Original language	English (Ireland)
Title of host publication	CIRCULATION
Publisher	LIPPINCOTT WILLIAMS & WILKINS
Number of pages	5
Volume	124
ISBN (Electronic)	0009-7322
ISBN (Print)	0009-7322
DOIs	https://doi.org/10.1161/CIRCULATIONAHA.110.012187
Publication status	Published - 1 Sep 2011

Authors (Note for portal: view the doc link for the full list of authors)

Authors
McLoughlin, D;McGuinness, J;Byrne, J;Terzo, E;Huuskonen, V;McAllister, H;Black, A;Kearney, S;Kay, E;Hill, ADK;Dietz, HC;Redmond, JM

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10.1161/CIRCULATIONAHA.110.012187

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@inproceedings{beff1cd672b24d5aa0bdd59ce2178a56,

title = "Pravastatin Reduces Marfan Aortic Dilation",

abstract = "Background-The sequelae of aortic root dilation are the lethal consequences of Marfan syndrome. The root dilation is attributable to an imbalance between deposition of matrix elements and metalloproteinases in the aortic medial layer as a result of excessive transforming growth factor-beta signaling. This study examined the efficacy and mechanism of statins in attenuating aortic root dilation in Marfan syndrome and compared effects to the other main proposed preventative agent, losartan.Methods and Results-Marfan mice heterozygous for a mutant allele encoding a cysteine substitution in fibrillin-1 (C1039G) were treated daily from 6 weeks old with pravastatin 0.5g L or losartan 0.6 g L. The end points of aortic root diameter (n = 25), aortic thickness, and architecture (n = 10), elastin volume (n = 5), dp dtmax (maximal rate of change of pressure) (cardiac catheter; n = 20), and ultrastructural analysis with stereology (electron microscopy; n = 5) were examined. The aortic root diameters of untreated Marfan mice were significantly increased in comparison to normal mice (0.161 + - 0.001 cm vs 0.252 + - 0.004 cm; P 0.01). Pravastatin (0.22 + - 0.003 cm; P 0.01) and losartan (0.221 + - 0.004 cm; P 0.01) produced a significant reduction in aortic root dilation. Both drugs also preserved elastin volume within the medial layer (pravastatin 0.23 + - 0.02 and losartan 0.29 + - 0.03 vs untreated Marfan 0.19 + - 0.02; P = 0.01; normal mice 0.27 + - 0.02). Ultrastructural analysis showed a reduction of rough endoplasmic reticulum in smooth muscle cells with pravastatin (0.022 + - 0.004) and losartan (0.013 + - 0.001) compared to untreated Marfan mice (0.035 + - 0.004; P 0.01).Conclusions-Statins are similar to losartan in attenuating aortic root dilation in a mouse model of Marfan syndrome. They appear to act through reducing the excessive protein manufacture by vascular smooth muscle cells, which occurs in the Marfan aorta. As a drug that is relatively well-tolerated for long-term use, it may be useful clinically. (Circulation. 2011; 124[suppl 1]: S168-S173.)",

author = "Alexander Black",

year = "2011",

month = sep,

day = "1",

doi = "10.1161/CIRCULATIONAHA.110.012187",

language = "English (Ireland)",

isbn = "0009-7322",

volume = "124",

booktitle = "CIRCULATION",

publisher = "LIPPINCOTT WILLIAMS & WILKINS",

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T1 - Pravastatin Reduces Marfan Aortic Dilation

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N2 - Background-The sequelae of aortic root dilation are the lethal consequences of Marfan syndrome. The root dilation is attributable to an imbalance between deposition of matrix elements and metalloproteinases in the aortic medial layer as a result of excessive transforming growth factor-beta signaling. This study examined the efficacy and mechanism of statins in attenuating aortic root dilation in Marfan syndrome and compared effects to the other main proposed preventative agent, losartan.Methods and Results-Marfan mice heterozygous for a mutant allele encoding a cysteine substitution in fibrillin-1 (C1039G) were treated daily from 6 weeks old with pravastatin 0.5g L or losartan 0.6 g L. The end points of aortic root diameter (n = 25), aortic thickness, and architecture (n = 10), elastin volume (n = 5), dp dtmax (maximal rate of change of pressure) (cardiac catheter; n = 20), and ultrastructural analysis with stereology (electron microscopy; n = 5) were examined. The aortic root diameters of untreated Marfan mice were significantly increased in comparison to normal mice (0.161 + - 0.001 cm vs 0.252 + - 0.004 cm; P 0.01). Pravastatin (0.22 + - 0.003 cm; P 0.01) and losartan (0.221 + - 0.004 cm; P 0.01) produced a significant reduction in aortic root dilation. Both drugs also preserved elastin volume within the medial layer (pravastatin 0.23 + - 0.02 and losartan 0.29 + - 0.03 vs untreated Marfan 0.19 + - 0.02; P = 0.01; normal mice 0.27 + - 0.02). Ultrastructural analysis showed a reduction of rough endoplasmic reticulum in smooth muscle cells with pravastatin (0.022 + - 0.004) and losartan (0.013 + - 0.001) compared to untreated Marfan mice (0.035 + - 0.004; P 0.01).Conclusions-Statins are similar to losartan in attenuating aortic root dilation in a mouse model of Marfan syndrome. They appear to act through reducing the excessive protein manufacture by vascular smooth muscle cells, which occurs in the Marfan aorta. As a drug that is relatively well-tolerated for long-term use, it may be useful clinically. (Circulation. 2011; 124[suppl 1]: S168-S173.)

AB - Background-The sequelae of aortic root dilation are the lethal consequences of Marfan syndrome. The root dilation is attributable to an imbalance between deposition of matrix elements and metalloproteinases in the aortic medial layer as a result of excessive transforming growth factor-beta signaling. This study examined the efficacy and mechanism of statins in attenuating aortic root dilation in Marfan syndrome and compared effects to the other main proposed preventative agent, losartan.Methods and Results-Marfan mice heterozygous for a mutant allele encoding a cysteine substitution in fibrillin-1 (C1039G) were treated daily from 6 weeks old with pravastatin 0.5g L or losartan 0.6 g L. The end points of aortic root diameter (n = 25), aortic thickness, and architecture (n = 10), elastin volume (n = 5), dp dtmax (maximal rate of change of pressure) (cardiac catheter; n = 20), and ultrastructural analysis with stereology (electron microscopy; n = 5) were examined. The aortic root diameters of untreated Marfan mice were significantly increased in comparison to normal mice (0.161 + - 0.001 cm vs 0.252 + - 0.004 cm; P 0.01). Pravastatin (0.22 + - 0.003 cm; P 0.01) and losartan (0.221 + - 0.004 cm; P 0.01) produced a significant reduction in aortic root dilation. Both drugs also preserved elastin volume within the medial layer (pravastatin 0.23 + - 0.02 and losartan 0.29 + - 0.03 vs untreated Marfan 0.19 + - 0.02; P = 0.01; normal mice 0.27 + - 0.02). Ultrastructural analysis showed a reduction of rough endoplasmic reticulum in smooth muscle cells with pravastatin (0.022 + - 0.004) and losartan (0.013 + - 0.001) compared to untreated Marfan mice (0.035 + - 0.004; P 0.01).Conclusions-Statins are similar to losartan in attenuating aortic root dilation in a mouse model of Marfan syndrome. They appear to act through reducing the excessive protein manufacture by vascular smooth muscle cells, which occurs in the Marfan aorta. As a drug that is relatively well-tolerated for long-term use, it may be useful clinically. (Circulation. 2011; 124[suppl 1]: S168-S173.)

U2 - 10.1161/CIRCULATIONAHA.110.012187

DO - 10.1161/CIRCULATIONAHA.110.012187

M3 - Conference Publication

SN - 0009-7322

VL - 124

BT - CIRCULATION

PB - LIPPINCOTT WILLIAMS & WILKINS

ER -

Pravastatin Reduces Marfan Aortic Dilation

Abstract

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