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神经聚集蛋白通过提高小鼠神经肌肉突触处的rapsyn蛋白水平,增加突触后乙酰胆碱受体的聚集。

Neural agrin increases postsynaptic ACh receptor packing by elevating rapsyn protein at the mouse neuromuscular synapse.

作者信息

Brockhausen Jennifer, Cole Rebecca N, Gervásio Othon L, Ngo Shyuan T, Noakes Peter G, Phillips William D

机构信息

School of Medical Sciences (Physiology), Bosch Institute, University of Sydney, Sydney, Australia.

出版信息

Dev Neurobiol. 2008 Aug;68(9):1153-69. doi: 10.1002/dneu.20654.

Abstract

Fluorescence resonance energy transfer (FRET) experiments at neuromuscular junctions in the mouse tibialis anterior muscle show that postsynaptic acetylcholine receptors (AChRs) become more tightly packed during the first month of postnatal development. Here, we report that the packing of AChRs into postsynaptic aggregates was reduced in 4-week postnatal mice that had reduced amounts of the AChR-associated protein, rapsyn, in the postsynaptic membrane (rapsyn(+/-) mice). We hypothesize that nerve-derived agrin increases postsynaptic expression and targeting of rapsyn, which then drives the developmental increase in AChR packing. Neural agrin treatment elevated the expression of rapsyn in C2 myotubes by a mechanism that involved slowing of rapsyn protein degradation. Similarly, exposure of synapses in postnatal muscle to exogenous agrin increased rapsyn protein levels and elevated the intensity of anti-rapsyn immunofluorescence, relative to AChR, in the postsynaptic membrane. This increase in the rapsyn-to-AChR immunofluorescence ratio was associated with tighter postsynaptic AChR packing and slowed AChR turnover. Acute blockade of synaptic AChRs with alpha-bungarotoxin lowered the rapsyn-to-AChR immunofluorescence ratio, suggesting that AChR signaling also helps regulate the assembly of extra rapsyn in the postsynaptic membrane. The results suggest that at the postnatal neuromuscular synapse agrin signaling elevates the expression and targeting of rapsyn to the postsynaptic membrane, thereby packing more AChRs into stable, functionally-important AChR aggregates.

摘要

对小鼠胫骨前肌神经肌肉接头处进行的荧光共振能量转移(FRET)实验表明,在出生后发育的第一个月,突触后乙酰胆碱受体(AChR)的聚集变得更加紧密。在此,我们报告称,在出生后4周的小鼠中,突触后膜中AChR相关蛋白rapsyn含量减少(rapsyn(+/-)小鼠),AChR聚集成突触后聚集体的情况减少。我们推测,神经源性聚集蛋白可增加rapsyn在突触后的表达和靶向定位,进而促使AChR聚集在发育过程中增加。神经聚集蛋白处理通过一种涉及减缓rapsyn蛋白降解的机制提高了C2肌管中rapsyn的表达。同样,将出生后肌肉中的突触暴露于外源性聚集蛋白下,相对于突触后膜中的AChR,rapsyn蛋白水平增加,抗rapsyn免疫荧光强度升高。rapsyn与AChR免疫荧光比率的这种增加与突触后AChR更紧密的聚集以及AChR周转减慢有关。用α-银环蛇毒素急性阻断突触AChR可降低rapsyn与AChR的免疫荧光比率,这表明AChR信号传导也有助于调节突触后膜中额外rapsyn的组装。结果表明,在出生后的神经肌肉突触处,聚集蛋白信号传导可提高rapsyn在突触后膜的表达和靶向定位,从而将更多的AChR聚集成稳定的、功能重要的AChR聚集体。

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