The Dynamic Nature of Coronary Artery Lesion Morphology Assessed by Serial Virtual Histology Intravascular Ultrasound Tissue Characterization

被引:283
|
作者
Kubo, Takashi [1 ]
Maehara, Akiko [1 ]
Mintz, Gary S. [1 ]
Doi, Hiroshi [1 ]
Tsujita, Kenichi [1 ]
Choi, So-Yeon [1 ]
Katoh, Osamu [2 ]
Nasu, Kenya [2 ]
Koenig, Andreas [3 ]
Pieper, Michael [4 ]
Rogers, Jason H. [5 ]
Wijns, William [6 ]
Boese, Dirk [7 ]
Margolis, Pauliina [8 ]
Moses, Jeffrey W. [1 ]
Stone, Gregg W. [1 ]
Leon, Martin B. [1 ]
机构
[1] Cardiovasc Res Fdn, New York, NY 10022 USA
[2] Toyohashi Heart Ctr, Aichi, Japan
[3] Univ Munich, Munich, Germany
[4] Herzzentrum Bodensee, Kreuzlingen, Switzerland
[5] Univ Calif Davis, Med Ctr, Sacramento, CA 95817 USA
[6] Onze Lieve Vrouw Hosp, Aalst, Belgium
[7] Univ Duisburg Essen, Essen, Germany
[8] Volcano Corp, San Diego, CA USA
关键词
atherosclerosis; coronary disease; intravascular ultrasound; virtual histology; RADIOFREQUENCY DATA-ANALYSIS; THIN-CAP FIBROATHEROMA; IN-VIVO; PLAQUE CLASSIFICATION; RUPTURED PLAQUES; DISEASE; CULPRIT; REPRODUCIBILITY; ANGIOGRAPHY; PROGRESSION;
D O I
10.1016/j.jacc.2009.07.078
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Objectives We used virtual histology intravascular ultrasound (VH-IVUS) to investigate the natural history of coronary artery lesion morphology. Background Plaque stability is related to its histological composition. Methods We performed serial (baseline and 12-month follow-up) VH-IVUS studies and examined 216 nonculprit lesions (plaque burden >= 40%) in 99 patients. Lesions were classified into pathological intimal thickening (PIT), VH-IVUS-derived thin-capped fibroatheroma (VH-TCFA), thick-capped fibroatheroma (ThCFA), fibrotic plaque, and fibrocalcific plaque. Results At baseline, 20 lesions were VH-TCFAs; during follow-up, 15 (75%) VH-TCFAs "healed," 13 became ThCFAs, 2 became fibrotic plaque, and 5 (25%) VH-TCFAs remained unchanged. Compared with VH-TCFAs that healed, VH-TCFAs that remained VH-TCFAs located more proximally (values are median [interquartile range]) (16 mm [15 to 18 mm] vs. 31 mm [22 to 47 mm], p = 0.013) and had larger lumen (9.1 mm(2) [8.2 to 10.7 mm(2)] vs. 6.9 mm(2) [6.0 to 8.2 mm(2)], p = 0.021), vessel (18.7 mm(2) [17.3 to 28.6 mm(2)] vs. 15.5 mm(2) [13.3 to 16.6 mm(2)]; p = 0.010), and plaque (9.7 mm(2) [9.6 to 15.7 mm(2)] vs. 8.4 mm(2) [7 to 9.7 mm(2)], p = 0.027) areas; however, baseline VH-IVUS plaque composition did not differ between VH-TCFAs that healed and VH-TCFAs that remained VH-TCFAs. Conversely, 12 new VH-TCFAs developed; 6 late-developing VH-TCFAs were PITs, and 6 were ThCFAs at baseline. In addition, plaque area at minimum lumen sites increased significantly in PITs (7.8 mm(2) [6.2 to 10.0 mm(2)] to 9.0 mm(2) [6.5 to 12.0 mm(2)], p < 0.001), VH-TCFAs (8.6 mm(2) [7.3 to 9.9 mm(2)] to 9.5 mm(2) [7.8 to 10.8 mm2], p = 0.024), and ThCFAs (8.6 mm(2) [6.8 to 10.2 mm(2)] to 8.8 mm(2) [7.1 to 11.4 mm(2)], p < 0.001) with a corresponding decrease lumen areas, but not in fibrous or fibrocalcific plaque. Conclusions Most VH-TCFAs healed during 12-month follow-up, whereas new VH-TCFAs also developed. PITs, VH-TCFAs, and ThCFAs showed significant plaque progression compared with fibrous and fibrocalcific plaque. (J Am Coll Cardiol 2010;55:1590-7) (C) 2010 by the American College of Cardiology Foundation
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收藏
页码:1590 / 1597
页数:8
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