It isn’t often that a single paper can change the way we think the brain works. But such is the case for the paper described in the previous post (full copy below *** ) if the implications I draw from it are correct.
Unfortunately this post requires a deep dive into neuroanatomy, neurophysiology, neuropharmacology and cellular molecular biology. I hope to put in enough background to make some of it comprehensible, but it is really written for the cognoscenti in these fields.
I’m pretty sure these thoughts are both original and unique
Briefly, the paper provided excellent evidence for one axon causing another to fire an impulse (an action potential). The fireror was from a neuron using acetyl choline as a neurotransmitter, and the fireree was a dopamine axon going to the striatum.
Dopamine axons are special. They go all over the brain. The cell body of the parent neuron of the axon to be synapsed on uses dopamine as a neurotransmitter. It sits in the pars compacta of the substantia nigra a fair piece away from the target they studied. “Individual neurons of the pars compact are calculated to give rise to 4.5 meters of axons once all the branches are summed” — [ Neuron vol. 96 p. 651 ’17 ].” These axons release dopamine all over the brain. There aren’t many dopamine neurons to begin with just 80,000 which is 1 millionth of the current (probably unreliable) estimate of the number of neurons in the brain 80,000,000,000.
Now synapses between neurons are easy to spot using electron microscopy. The presynaptic terminal contains a bunch of small vesicles and is closely apposed (300 Angstroms — way below anything the our eyes can see) to the post synaptic neuron which also looks different, usually having a density just under the membrane (called, logically enough, post-synaptic density). Embedded in the postsynaptic membrane are proteins which conduct ions such as Na+, K+, Cl- into the postsynaptic neuron triggering an action potential.
But the dopamine axons going all over the brain have a lot of presynaptic specialization, but the post-synaptic neuron and its postsynaptic density is nowhere to be found. This is called volume neurotransmission.
The story doesn’t end with dopamine. There are 3 other similar systems of small numbers of neurons collected into nuclei, using different neurotransmitters, but whose axons branch and branch so they go all over the brain.
These are the locus coeruleus which uses norepinephrine as a neurotransmitter, the dorsal raphe nucleus which uses serotonin and the basal nucleus of Meynert which uses acetyl choline.
What is so remarkable about the paper, that it allows the receiving neurons to (partially) control what dopamine input it gets.
But dopamine doesn’t work at the synapse, and the 5 receptors for it (called G Protein Coupled Receptors — GPCRs) aren’t found there. None of the GPCRs conduct ions or trigger action potentials (immediately anyway). Instead, they produce their effects much more slowly and change the metabolism of the interior of the cell.
Neither does norepinephrine all of whose receptors are GPCRs. Serotonin does have one of its 16 or so receptors which conducts ions, but the rest are GPCRs.
Acetyl choline does have one class of receptors (nicotinic) which conducts ions, and which the paper shows is what is triggering the axon on axon synapse. The other class (muscarinic) of acetyl choline receptor is a GPCR.
We do know that the norepinephrine and serotonin axons work by volume neurotransmission (not sure about those of the basal nucleus of Meynert).
Now the paper tested axon to axon firing in one of the four systems (dopamine) in one of the places its axons goes (the striatum). There is no question that the axons of all 4 systems ramify widely.
Suppose axon to axon firing is general, so a given region can control in someway how much dopamine/serotonin/norepinephrine/acetyl choline it is getting.
Does this remind you of any system you are familiar with? Maybe, because my wife went to architecture school, it reminds me of an old apartment building, with separate systems to distribute electricity, plumbing, steam heat and water to each apartment, which controls how much of each it gets.
Perhaps these four systems are basically neurological utilities, necessary for the function of the brain, but possibly irrelevant to the computations it is carrying out, like a mother heating a bottle for her baby in water on a gas stove on a cold winter night. The nature of steam heat, electricity, water and gas tell you very little about what is going on in her apartment.
The paper is so new (the Neuron issue of 21 September) that more implications are sure to present themselves.
Quibbles are sure to arise. One is that fact that the gray matter of our brain doesn’t contain much in the way of neurons using acetyl choline as a neurotransmitter. What it does have is lots of neurons using GABA which we know can act on axons, inhibiting axon potential generation. This has been well worked out with synapses where the axon emerges from the neuron cell body (the initial segment).
The work was done in living animals, so no microscopy is available showing the synapse. Such work is sure to be done. No classical presynaptic apparatus may be present, just two naked axons touching each other and interacting by ephaptic transmission.
So a lot of work should be done, the first of which should be replication. As the late Carl Sagan said “extraordinary claims require extraordinary evidence”.
Finally:
As Mark Twain said ” There is something fascinating about science. One gets such wholesale returns of conjecture out of such a trifling investment of fact.”
Chemiotics II 