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肝微粒体对钙的摄取机制:阴离子和离子载体的作用。

The mechanism of calcium uptake by liver microsomes: effect of anions and ionophores.

作者信息

Chan K M, Koepnick S L

出版信息

Biochim Biophys Acta. 1985 Sep 10;818(3):291-8. doi: 10.1016/0005-2736(85)90002-1.

Abstract

The mechanism of calcium uptake by liver microsomes was investigated using various anions and ionophores. Calcium uptake was shown to be specific to microsomes and unlikely to be due to contamination by plasma membranes by correlation of calcium uptake to the marker enzymes specific for these two fractions. Under the conditions employed, phosphates, sulfate, chloride, acetate, nitrate, thiocyanate, maleate, succinate and oxalate all stimulated calcium uptake by microsomes, but to different degrees. The greatest effect (4-6-fold) was observed with phosphate. On the contrary, phosphate is the only anion that stimulates the plasma membrane calcium uptake to any significant degree. Treatment of isolated microsomes with 4,4'-diisothiocyano-2,2'-disulfonic acid stilbene (DIDS) resulted in inhibition of ATP- and anion-dependent calcium uptake. A lipid-permeable organic acid such as maleate retained its ability to promote calcium uptake in DIDS-treated microsomes. However, a lipophilic anion, such as nitrate, stimulated calcium uptake only in the presence of the protonophore carbonyl cyanide m-chlorophenylhydrazone (CCCP). In addition, 2 microM valinomycin, when added in the absence or presence of 10 to 100 mM K+, had no stimulatory effect on calcium uptake. These results appear to be consistent with a model in which the active uptake of calcium into microsomes involves electroneutral Ca2+-nH+ exchange.

摘要

利用各种阴离子和离子载体研究了肝微粒体对钙的摄取机制。通过将钙摄取与这两个组分特有的标记酶进行关联,结果表明钙摄取对微粒体具有特异性,不太可能是由于质膜污染所致。在所采用的条件下,磷酸盐、硫酸盐、氯化物、乙酸盐、硝酸盐、硫氰酸盐、马来酸盐、琥珀酸盐和草酸盐均能刺激微粒体对钙的摄取,但程度不同。磷酸盐的刺激作用最大(4至6倍)。相反,磷酸盐是唯一能在任何显著程度上刺激质膜钙摄取的阴离子。用4,4'-二异硫氰酸-2,2'-二磺酸芪(DIDS)处理分离的微粒体导致ATP和阴离子依赖性钙摄取受到抑制。一种脂溶性有机酸如马来酸盐在DIDS处理的微粒体中仍保留促进钙摄取的能力。然而,一种亲脂性阴离子如硝酸盐仅在质子载体羰基氰化物间氯苯腙(CCCP)存在时刺激钙摄取。此外,2 microM缬氨霉素在不存在或存在10至100 mM K+的情况下添加时,对钙摄取没有刺激作用。这些结果似乎与一种模型一致,即钙主动摄取到微粒体中涉及电中性的Ca2+-nH+交换。

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