Besse S, Delcayre C, Chevalier B, Hardouin S, Heymes C, Bourgeois F, Moalic J M, Swynghedauw B
Unité 127-INSERM, Hôpital Lariboisière, Paris, France.
Cardiovasc Drugs Ther. 1994 Aug;8(4):581-7. doi: 10.1007/BF00877412.
Heart failure mainly occurs during the last decades of life, and it is important to know if the senescent heart is not an already failing heart. During aging, both contraction and relaxation of papillary muscle are impaired. Such an impairment is compensated in vivo and the cardiac output remains normal. In spite of a loss in myocytes, the heart weight/body weight ratio is unchanged, but the myocytes are bigger. Arrhythmias are permanent and are accompanied by a loss of the normal heart rate variability. Changes in specific mRNAs include: a shift in myosin heavy chain (MHC) isogene expression leading to an increased beta MHC content; decreased densities of Ca2+ ATPase of the sarcoplasmic reticulum, beta 1-adrenergic receptor, and muscarinic receptors; and attenuation of the Na+/Ca2+ exchange activity. Most of these changes, but not all, resemble those observed during cardiac overload and are accompanied by an increased duration of both the action potential and the intracellular calcium transient. However, the senescent heart is still able to further modify its phenotype in response to mechanical overload. The senescent heart is a diseased heart, and the origin of the "disease" is multifactorial and includes the general process of senescence, hormonal changes, and the myocardial consequences of senescence of the vessels.
心力衰竭主要发生在生命的最后几十年,了解衰老的心脏是否并非已经处于衰竭状态很重要。在衰老过程中,乳头肌的收缩和舒张功能都会受损。这种损害在体内会得到代偿,心输出量保持正常。尽管心肌细胞有所减少,但心脏重量与体重之比不变,不过心肌细胞会更大。心律失常持续存在,并伴有正常心率变异性的丧失。特定mRNA的变化包括:肌球蛋白重链(MHC)同工基因表达发生转变,导致β-MHC含量增加;肌浆网Ca2+ATP酶、β1-肾上腺素能受体和毒蕈碱受体的密度降低;以及Na+/Ca2+交换活性减弱。这些变化中的大多数(但并非全部)与心脏负荷过重时观察到的变化相似,并伴有动作电位和细胞内钙瞬变持续时间的增加。然而,衰老的心脏仍能够响应机械负荷进一步改变其表型。衰老的心脏是患病的心脏,“疾病”的起源是多因素的,包括衰老的一般过程、激素变化以及血管衰老对心肌的影响。
