Scheiderer Cary L, McCutchen Eve, Thacker Erin E, Kolasa Krystyna, Ward Matthew K, Parsons Dee, Harrell Lindy E, Dobrunz Lynn E, McMahon Lori L
Department Neurobiology, University of Alabama, Birmingham, Alabama 35294, USA.
J Neurosci. 2006 Apr 5;26(14):3745-56. doi: 10.1523/JNEUROSCI.5507-05.2006.
Degeneration of septohippocampal cholinergic neurons results in memory deficits attributable to loss of cholinergic modulation of hippocampal synaptic circuits. A remarkable consequence of cholinergic degeneration is the sprouting of noradrenergic sympathetic fibers from the superior cervical ganglia into hippocampus. The functional impact of sympathetic ingrowth on synaptic physiology has never been investigated. Here, we report that, at CA3-CA1 synapses, a Hebbian form of long-term depression (LTD) induced by muscarinic M1 receptor activation (mLTD) is lost after medial septal lesion. Unexpectedly, expression of mLTD is rescued by sympathetic sprouting. These effects are specific because LTP and other forms of LTD are unaffected. The rescue of mLTD expression is coupled temporally with the reappearance of cholinergic fibers in hippocampus, as assessed by the immunostaining of fibers for VAChT (vesicular acetylcholine transporter). Both the cholinergic reinnervation and mLTD rescue are prevented by bilateral superior cervical ganglionectomy, which also prevents the noradrenergic sympathetic sprouting. The new cholinergic fibers likely originate from the superior cervical ganglia because unilateral ganglionectomy, performed when cholinergic reinnervation is well established, removes the reinnervation on the ipsilateral side. Thus, the temporal coupling of the cholinergic reinnervation with mLTD rescue, together with the absence of reinnervation and mLTD expression after ganglionectomy, demonstrate that the autonomic-driven cholinergic reinnervation is essential for maintaining mLTD after central cholinergic cell death. We have discovered a novel phenomenon whereby the autonomic and central nervous systems experience structural rearrangement to replace lost cholinergic innervation in hippocampus, with the consequence of preserving a form of LTD that would otherwise be lost as a result of cholinergic degeneration.
隔海马胆碱能神经元的退变导致记忆缺陷,这归因于海马突触回路胆碱能调节的丧失。胆碱能退变的一个显著后果是颈上神经节的去甲肾上腺素能交感纤维向海马内生长。交感神经纤维长入对突触生理学的功能影响从未被研究过。在此,我们报告,在CA3-CA1突触处,毒蕈碱M1受体激活诱导的一种赫布形式的长时程抑制(LTD)(mLTD)在内侧隔区损伤后消失。出乎意料的是,交感神经纤维的生长挽救了mLTD的表达。这些效应是特异性的,因为长时程增强(LTP)和其他形式的LTD不受影响。通过对囊泡乙酰胆碱转运体(VAChT)进行纤维免疫染色评估,mLTD表达的挽救在时间上与海马中胆碱能纤维的重新出现相关。双侧颈上神经节切除术可阻止胆碱能神经再支配和mLTD的挽救,这也能阻止去甲肾上腺素能交感神经纤维的生长。新的胆碱能纤维可能起源于颈上神经节,因为在胆碱能神经再支配充分建立后进行单侧神经节切除术,可去除同侧的神经再支配。因此,胆碱能神经再支配与mLTD挽救在时间上的关联,以及神经节切除术后神经再支配和mLTD表达的缺失,表明自主神经驱动的胆碱能神经再支配对于中枢胆碱能细胞死亡后维持mLTD至关重要。我们发现了一种新现象,即自主神经系统和中枢神经系统经历结构重排,以取代海马中丧失的胆碱能神经支配,结果是保留了一种LTD形式,否则这种LTD会因胆碱能退变而丧失。