de Jong Hendrik, Neal Andrea C, Coleman Rosalind A, Lewin Tal M
Department of Nutrition, University of North Carolina at Chapel Hill, CB# 7461, NC 27599, USA.
Biochim Biophys Acta. 2007 Jan;1771(1):75-82. doi: 10.1016/j.bbalip.2006.11.007. Epub 2006 Nov 30.
Long-chain acyl-CoA synthetases (ACSL) activate fatty acids (FA) and provide substrates for virtually every metabolic pathway that catabolizes FA or synthesizes complex lipids. We have hypothesized that each of the five cloned ACSL isoforms partitions FA towards specific downstream pathways. Adult heart expresses all five cloned ACSL isoforms, but their independent functional roles have not been elucidated. Studies implicate ACSL1 in both oxidative and lipid synthetic pathways. To clarify the functional role of ACSL1 and the other ACSL isoforms (3-6), we examined ACS specific activity and Acsl mRNA expression in the developing mouse heart which increases FA oxidative pathways for energy production after birth. Compared to the embryonic heart, ACS specific activity was 14-fold higher on post-natal day 1 (P1). On P1, as compared to the fetus, only Acsl1 mRNA increased, whereas transcripts for the other Acsl isoforms remained the same, suggesting that ACSL1 is the major isoform responsible for activating long-chain FA for myocardial oxidation after birth. In contrast, the mRNA abundance of Acsl3 was highest on E16, and decreased dramatically by P7, suggesting that ACSL3 may play a critical role during the development of the fetal heart. Our data support the hypothesis that each ACSL has a specific role in the channeling of FA towards distinct metabolic fates.
长链脂酰辅酶A合成酶(ACSL)激活脂肪酸(FA),并为几乎每一条分解代谢FA或合成复合脂质的代谢途径提供底物。我们推测,五个已克隆的ACSL亚型各自将FA导向特定的下游途径。成年心脏表达所有五个已克隆的ACSL亚型,但其独立的功能作用尚未阐明。研究表明ACSL1参与氧化和脂质合成途径。为了阐明ACSL1和其他ACSL亚型(3 - 6)的功能作用,我们检测了发育中的小鼠心脏中的ACSL比活性和Acsl mRNA表达,出生后小鼠心脏会增加FA氧化途径以产生能量。与胚胎心脏相比,出生后第1天(P1)的ACSL比活性高14倍。在P1时,与胎儿相比,只有Acsl1 mRNA增加,而其他Acsl亚型的转录本保持不变,这表明ACSL1是出生后激活长链FA用于心肌氧化的主要亚型。相反,Acsl3的mRNA丰度在胚胎第16天(E16)时最高,并在出生后第7天(P7)急剧下降,这表明ACSL3可能在胎儿心脏发育过程中起关键作用。我们的数据支持这样的假设,即每个ACSL在将FA导向不同代谢命运的过程中都有特定作用。