Tahiliani A G, Beinlich C J
Geisinger Clinic, Weis Center for Research, Danville, Pennsylvania 17822.
Vitam Horm. 1991;46:165-228. doi: 10.1016/s0083-6729(08)60684-6.
In summary, the vitamin pantothenic acid is an integral part of the acylation carriers, CoA and acyl carrier protein (ACP). The vitamin is readily available from diverse dietary sources, a fact which is underscored by the difficulty encountered in attempting to induce pantothenate deficiency. Although pantothenic acid deficiency has not been linked with any particular disease, deficiency of the vitamin results in generalized malaise clinically. In view of the fact that pantothenate is required for the synthesis of CoA, it is surprising that tissue CoA levels are not altered in pantothenate deficiency. This suggests that the cell is equipped to conserve its pantothenate content, possibly by a recycling mechanism for utilizing pantothenate obtained from degradation of pantothenate-containing molecules. Although the steps involved in the conversion of pantothenate to CoA have been characterized, much remains to be done to understand the regulation of CoA synthesis. In particular, in view of what is known about the in vitro regulation of pantothenate kinase, it is surprising that the enzyme is active in vivo, since factors that are known to inhibit the enzyme are present in excess of the concentrations known to inhibit the enzyme. Thus, other physiological regulatory factors (which are largely unknown) must counteract the effects of these inhibitors, since the pantothenate-to-CoA conversion is operative in vivo. Another step in the biosynthetic pathway that may be rate limiting is the conversion of 4'-phosphopantetheine (4'-PP) to dephospho-CoA, a step catalyzed by 4'-phosphopantetheine adenylyl-transferase. In mammalian systems, this step may occur in the mitochondria or in the cytosol. The teleological significance of these two pathways remains to be established, particularly since mitochondria are capable of transporting CoA from the cytosol. Altered homeostasis of CoA has been observed in diverse disease states including starvation, diabetes, alcoholism, Reye syndrome (RS), medium-chain acyl CoA dehydrogenase deficiency, vitamin B12 deficiency, and certain tumors. Hormones, such as glucocorticoids, insulin, and glucagon, as well as drugs, such as clofibrate, also affect tissue CoA levels. It is not known whether the abnormal metabolism observed in these conditions is the result of altered CoA metabolism or whether CoA levels change in response to hormonal or nonhormonal perturbations brought about in these conditions. In other words, a cause-effect relation remains to be elucidated. It is also not known whether the altered CoA metabolism (be it cause or result of abnormal metabolism) can be implicated in the manifestations of a disease. Besides CoA, pantothenic acid is also an integral part of the ACP molecule.(ABSTRACT TRUNCATED AT 400 WORDS)
总之,维生素泛酸是酰化载体辅酶A(CoA)和酰基载体蛋白(ACP)不可或缺的组成部分。该维生素可从多种饮食来源轻易获取,这一事实因试图诱发泛酸缺乏时遇到的困难而得到凸显。尽管泛酸缺乏尚未与任何特定疾病相关联,但临床上维生素缺乏会导致全身不适。鉴于合成CoA需要泛酸,令人惊讶的是,泛酸缺乏时组织CoA水平并未改变。这表明细胞具备保存其泛酸含量的能力,可能是通过一种循环机制来利用从含泛酸分子降解中获得的泛酸。尽管泛酸转化为CoA所涉及的步骤已得到表征,但要理解CoA合成的调控仍有许多工作要做。特别是,鉴于已知的泛酸激酶体外调控情况,该酶在体内具有活性这一点令人惊讶,因为已知抑制该酶的因子其存在浓度超过已知的抑制浓度。因此,其他生理调节因子(大多未知)必定会抵消这些抑制剂的作用,因为泛酸到CoA的转化在体内是有效的。生物合成途径中另一个可能限速的步骤是4'-磷酸泛酰巯基乙胺(4'-PP)转化为脱磷酸CoA,这一步由4'-磷酸泛酰巯基乙胺腺苷酰转移酶催化。在哺乳动物系统中,这一步可能发生在线粒体或细胞质中。这两条途径的目的论意义仍有待确定,特别是因为线粒体能够从细胞质转运CoA。在多种疾病状态下已观察到CoA稳态的改变,包括饥饿、糖尿病、酒精中毒、瑞氏综合征(RS)、中链酰基辅酶A脱氢酶缺乏症、维生素B12缺乏症以及某些肿瘤。激素,如糖皮质激素、胰岛素和胰高血糖素,以及药物,如氯贝丁酯,也会影响组织CoA水平。尚不清楚在这些情况下观察到的异常代谢是CoA代谢改变的结果,还是CoA水平因这些情况下发生的激素或非激素扰动而发生变化。换句话说,因果关系仍有待阐明。也不清楚CoA代谢的改变(无论是异常代谢的原因还是结果)是否与疾病表现有关。除了CoA,泛酸也是ACP分子不可或缺的组成部分。(摘要截断于400字)
