Farrar W L, Brini A T, Harel-Bellan A, Korner M, Ferris D K
National Cancer Institute-Frederick Cancer Research Facility, Maryland.
Immunol Ser. 1990;49:379-410.
Hemopoietic cells have an absolute requirement for survival and proliferation for specific growth factors. The growth factors maintain the critical vitality of the cells by stimulating adenosine triphosphate (ATP) synthesis and hexose transport. Intracellular alkalinization also occurs rapidly through the stimulation of the Na+/H+ antiporter. These immediate metabolic events, not initiated by serum components, appear to be necessary for the integrity of cellular viability (Fig. 6). Interleukin-3 has been shown to induce the activation of PK-C through a mechanism(s) not requiring the hydrolysis of phosphoinositol 4,5 bisphosphate. A role for Ca2+ influx or intracellular release in the action of CSFs or interleukins has not been shown. Although downregulation of cAMP has been reported in response to IL-2, the signal transduction process of CSFs and IL-2 appears not to be mediated by upregulation of cyclic nucleotide metabolism or "classical" phospholipid degradative pathways. Protein phosphorylation is clearly modulated by the hemopoietic cytokines, yet only the CSF-1 receptor has any known intrinsic kinase activity. Instead, the IL-3, GM-CSF receptors, and perhaps G-CSF appear to be coupling to kinases of both tyrosine and serine specificities. This may be a direct allosteric interaction with membrane-associated kinases or transduced through an intermediate protein such as those using GTP. Such is the case for many hormone receptors that couple to amplifying "second messenger" enzyme systems (i.e., adenylate cyclase, phospholipase C) or members of the insulin growth factor family that couple to tyrosine kinases in proximity to the receptors (IGF-II). One of the kinase systems that IL-2, IL-3, and other CSFs stimulate appears to have some characteristics similar to PK-C. Direct activators of PK-C stimulate some similar serine-threonine phosphorylation and perhaps even tyrosine phosphorylation. The hemopoietic growth factors, however, stimulate tyrosine phosphorylation of some proteins that are not phosphorylated in response to PK-C activators, suggesting that these kinase systems are independently regulated. Although phorbol esters stimulate many of the same metabolic activities (ATP synthesis in myeloid and lymphoid cell lines), growth-factor abrogation is clearly associated with the action of tyrosine kinase oncogenes or the nuclear oncogene effectors such as v-myc. It is likely, therefore, that tyrosine kinases are playing a critical role in the control of proliferation although the dominant amount of cellular protein phosphorylations are on serine. Both classes of kinases are apparently required for growth-factor action. All the hemopoietic growth factors examined thus far stimulate the steady-state accumulation of the nuclear protooncogenes.(ABSTRACT TRUNCATED AT 400 WORDS)
造血细胞的存活和增殖绝对需要特定的生长因子。这些生长因子通过刺激三磷酸腺苷(ATP)合成和己糖转运来维持细胞的关键活力。通过刺激Na+/H+反向转运体,细胞内也会迅速发生碱化。这些并非由血清成分引发的即时代谢事件,似乎对细胞活力的完整性是必需的(图6)。白细胞介素-3已被证明可通过一种不需要磷酸肌醇4,5-二磷酸水解的机制诱导蛋白激酶C(PK-C)的激活。尚未证明Ca2+内流或细胞内释放在集落刺激因子(CSF)或白细胞介素的作用中有作用。尽管有报道称白细胞介素-2可导致环磷酸腺苷(cAMP)下调,但CSF和白细胞介素-2的信号转导过程似乎不是由环核苷酸代谢上调或“经典”磷脂降解途径介导的。造血细胞因子明显调节蛋白磷酸化,但只有CSF-1受体具有任何已知的内在激酶活性。相反,白细胞介素-3、粒细胞-巨噬细胞集落刺激因子(GM-CSF)受体,可能还有粒细胞集落刺激因子(G-CSF)受体,似乎与酪氨酸和丝氨酸特异性的激酶偶联。这可能是与膜相关激酶的直接变构相互作用,或者是通过一种中间蛋白转导的,比如那些利用鸟苷三磷酸(GTP)的蛋白。许多与放大的“第二信使”酶系统(即腺苷酸环化酶、磷脂酶C)偶联的激素受体,或者与受体附近的酪氨酸激酶偶联的胰岛素生长因子家族成员(胰岛素样生长因子-II)就是这种情况。白细胞介素-2、白细胞介素-3和其他CSF刺激的一种激酶系统似乎具有一些与PK-C相似的特征。PK-C的直接激活剂刺激一些类似的丝氨酸-苏氨酸磷酸化,甚至可能刺激酪氨酸磷酸化。然而,造血生长因子刺激一些蛋白的酪氨酸磷酸化,而这些蛋白在PK-C激活剂作用下不会被磷酸化,这表明这些激酶系统是独立调节的。尽管佛波酯刺激许多相同的代谢活动(骨髓和淋巴细胞系中的ATP合成),但生长因子的消除显然与酪氨酸激酶癌基因或核癌基因效应物(如v-myc)的作用有关。因此,酪氨酸激酶可能在增殖控制中起关键作用,尽管细胞蛋白磷酸化的主要部分是在丝氨酸上。这两类激酶显然都是生长因子作用所必需的。迄今为止所检测的所有造血生长因子都刺激核原癌基因的稳态积累。(摘要截选至400字)
