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cAMP 介导的培养的大鼠垂体泌乳素细胞融合孔的稳定化。

cAMP-mediated stabilization of fusion pores in cultured rat pituitary lactotrophs.

机构信息

Centre for Environmental and Marine Studies, Departamento de Biologia, Universidade de Aveiro, 3810-193 Aveiro, Portugal.

出版信息

J Neurosci. 2013 May 1;33(18):8068-78. doi: 10.1523/JNEUROSCI.5351-12.2013.

Abstract

Regulated exocytosis mediates the release of hormones and transmitters. The last step of this process is represented by the merger between the vesicle and the plasma membranes, and the formation of a fusion pore. Once formed, the initially stable and narrow fusion pore may reversibly widen (transient exocytosis) or fully open (full-fusion exocytosis). Exocytosis is typically triggered by an elevation in cytosolic calcium activity. However, other second messengers, such as cAMP, have been reported to modulate secretion. The way in which cAMP influences the transitions between different fusion pore states remains unclear. Here, hormone release studies show that prolactin release from isolated rat lactotrophs stimulated by forskolin, an activator of adenylyl cyclases, and by membrane-permeable cAMP analog (dbcAMP), exhibit a biphasic concentration dependency. Although at lower concentrations (2-10 μm forskolin and 2.5-5 mm dbcAMP) these agents stimulate prolactin release, an inhibition is measured at higher concentrations (50 μm forskolin and 10-15 mm dbcAMP). By using high-resolution capacitance (Cm) measurements, we recorded discrete increases in Cm, which represent elementary exocytic events. An elevation of cAMP leaves the frequency of full-fusion events unchanged while increasing the frequency of transient events. These exhibited a wider fusion pore as measured by increased fusion pore conductance and a prolonged fusion pore dwell time. The probability of observing rhythmic reopening of transient fusion pores was elevated by dbcAMP. In conclusion, cAMP-mediated stabilization of wide fusion pores prevents vesicles from proceeding to the full-fusion stage of exocytosis, which hinders vesicle content discharge at high cAMP concentrations.

摘要

受调控的胞吐作用介导激素和递质的释放。该过程的最后一步由囊泡与质膜融合以及融合孔的形成来代表。一旦形成,最初稳定且狭窄的融合孔可能会可逆地扩张(瞬时胞吐作用)或完全打开(完全融合胞吐作用)。胞吐作用通常由细胞溶质钙离子活性的升高触发。然而,已经报道其他第二信使,如 cAMP,可调节分泌。cAMP 影响不同融合孔状态之间转变的方式仍不清楚。在这里,激素释放研究表明,由福斯柯林(一种腺苷酸环化酶激活剂)和膜可渗透的 cAMP 类似物(dbcAMP)刺激的分离大鼠催乳素细胞中催乳素的释放表现出双相浓度依赖性。尽管在较低浓度(2-10μm 福斯柯林和 2.5-5mm dbcAMP)下,这些试剂刺激催乳素释放,但在较高浓度(50μm 福斯柯林和 10-15mm dbcAMP)下测量到抑制作用。通过使用高分辨率电容(Cm)测量,我们记录了 Cm 的离散增加,这代表基本的胞吐作用事件。cAMP 的升高使完全融合事件的频率保持不变,同时增加了瞬时事件的频率。这些事件表现出更宽的融合孔,如通过增加融合孔电导和延长融合孔停留时间来测量。dbcAMP 提高了观察到瞬时融合孔有节奏重新开放的概率。总之,cAMP 介导的宽融合孔的稳定作用阻止了囊泡进入胞吐作用的完全融合阶段,这阻碍了在高 cAMP 浓度下囊泡内容物的释放。

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