Comparative specialization of intrinsic cardiac neurons in humans, mice, and pigs.
John D TompkinsDonald B HooverLeif A HavtonJanaki C PatelYoungjin ChoElizabeth H SmithNatalia P BiscolaOlujimi A AjijolaKalyanam ShivkumarJeffrey L ArdellPublished in: bioRxiv : the preprint server for biology (2024)
Intrinsic cardiac neurons (ICNs) play a crucial role in the proper functioning of the heart; yet a paucity of data pertaining to human ICNs exists. We took a multidisciplinary approach to complete a detailed cellular comparison of the structure and function of ICNs from mice, pigs, and humans. Immunohistochemistry of whole and sectioned ganglia, transmission electron microscopy, intracellular microelectrode recording and dye filling for quantitative morphometry were used to define the neurophysiology, histochemistry, and ultrastructure of these cells across species. The densely packed, smaller ICNs of mouse lacked dendrites, formed axosomatic connections, and had high synaptic efficacy constituting an obligatory synapse. At Pig ICNs, a convergence of subthreshold cholinergic inputs onto extensive dendritic arbors supported greater summation and integration of synaptic input. Human ICNs were tonically firing, with synaptic stimulation evoking large suprathreshold excitatory postsynaptic potentials like mouse, and subthreshold potentials like pig. Ultrastructural examination of synaptic terminals revealed conserved architecture, yet small clear vesicles (SCVs) were larger in pigs and humans. The presence and localization of ganglionic neuropeptides was distinct, with abundant VIP observed in human but not pig or mouse ganglia, and little SP or CGRP in pig ganglia. Action potential waveforms were similar, but human ICNs had larger after-hyperpolarizations. Intrinsic excitability differed; 93% of human cells were tonic, all pig neurons were phasic, and both phasic and tonic phenotypes were observed in mouse. In combination, this publicly accessible, multimodal atlas of ICNs from mice, pigs, and humans identifies similarities and differences in the evolution of ICNs.
Keyphrases
- endothelial cells
- induced pluripotent stem cells
- electron microscopy
- pluripotent stem cells
- spinal cord
- left ventricular
- type diabetes
- heart failure
- adipose tissue
- induced apoptosis
- transcription factor
- metabolic syndrome
- mass spectrometry
- atrial fibrillation
- prefrontal cortex
- cell proliferation
- endoplasmic reticulum stress