Hsieh Patrick C H, MacGillivray Catherine, Gannon Joseph, Cruz Francisco U, Lee Richard T
Cardiovascular Division, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, Cambridge, Mass., USA.
Circulation. 2006 Aug 15;114(7):637-44. doi: 10.1161/CIRCULATIONAHA.106.639831. Epub 2006 Aug 7.
Local delivery methods can target therapies to specific tissues and potentially avoid toxicity to other organs. Platelet-derived growth factor can protect the myocardium, but it also plays an important role in promoting pulmonary hypertension. It is not known whether local myocardial delivery of platelet-derived growth factor during myocardial infarction (MI) can lead to sustained cardiac benefit without causing pulmonary hypertension.
We performed a randomized and blinded experiment of 127 rats that survived experimental MI or sham surgery. We delivered platelet-derived growth factor (PDGF)-BB with self-assembling peptide nanofibers (NFs) to provide controlled release within the myocardium. There were 6 groups with n > or = 20 in each group: sham, sham+NF, sham+NF/PDGF, MI, MI+NF, and MI+NF/PDGF. Serial echocardiography from 1 day to 3 months showed significant improvement of ventricular fractional shortening, end-systolic dimension, and end-diastolic dimension with local PDGF delivery (P < 0.05 for MI+NF/PDGF versus MI or MI+NF). Catheterization at 4 months revealed improved ventricular function in the controlled delivery group (left ventricular end-diastolic pressure, cardiac index, +dP/dt, -dP/dt, and time constant of exponential decay all P < 0.05 for MI+NF/P versus MI or MI+NF). Infarcted myocardial volume was reduced by NF/PDGF therapy (34.0 +/- 13.3% in MI, 28.9 +/- 12.9% in MI+NF, and 12.0 +/- 5.8% in MI+NF/PDGF; P < 0.001). There was no evidence of pulmonary toxicity from the therapy, with no differences in right ventricular end-systolic pressure, right ventricular dP/dt, bromodeoxyuridine staining, or pulmonary artery medial wall thickness.
Intramyocardial delivery of PDGF by self-assembling peptide NFs leads to long-term improvement in cardiac performance after experimental infarction without apparent pulmonary toxicity. Local myocardial protection may allow prevention of heart failure without systemic toxicity.
局部给药方法可将治疗靶向特定组织,并有可能避免对其他器官产生毒性。血小板衍生生长因子可保护心肌,但它在促进肺动脉高压方面也起重要作用。目前尚不清楚在心肌梗死(MI)期间局部心肌递送血小板衍生生长因子是否能在不引起肺动脉高压的情况下带来持续的心脏益处。
我们对127只在实验性MI或假手术后存活的大鼠进行了一项随机双盲实验。我们将血小板衍生生长因子(PDGF)-BB与自组装肽纳米纤维(NFs)一起递送,以在心肌内实现控释。共有6组,每组n≥20只:假手术组、假手术+NF组、假手术+NF/PDGF组、MI组、MI+NF组和MI+NF/PDGF组。从1天到3个月的系列超声心动图显示,局部递送PDGF可使心室缩短分数、收缩末期内径和舒张末期内径有显著改善(MI+NF/PDGF组与MI组或MI+NF组相比,P<0.05)。4个月时的导管检查显示,控释组的心室功能有所改善(左心室舒张末期压力、心脏指数、+dP/dt、-dP/dt以及指数衰减时间常数,MI+NF/P组与MI组或MI+NF组相比,均P<0.05)。NF/PDGF治疗可减少梗死心肌体积(MI组为34.0±13.3%,MI+NF组为28.9±12.9%,MI+NF/PDGF组为12.0±5.8%;P<0.001)。没有证据表明该治疗存在肺毒性,右心室收缩末期压力、右心室dP/dt、溴脱氧尿苷染色或肺动脉中膜厚度均无差异。
通过自组装肽NFs进行心肌内递送PDGF可使实验性梗死后的心脏功能长期改善,且无明显肺毒性。局部心肌保护可能允许预防心力衰竭而无全身毒性。
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