Abstract
The title usage of Latin Quo vadis ‘where are you going’ extends the
question Unde venisti from where ‘did you come?’ posed in the
accompanying paper and extends consideration of how ancient eukaryotic and
eumetazoan functions of progesterone receptor membrane component (PGRMC) proteins
(PGRMC1 and PGRMC2 in mammals) could influence modern human health and disease.
This paper attempts to extrapolate to modern biology in terms of extensions of
hypothetical ancestral functional states from early eukaryotes and the last
eumetazoan common ancestor (LEUMCA), to relativize human metabolic physiology and
disease. As novel cell types and functional specializations appeared in
bilaterian animals, PGRMC functions are hypothesized to have continued to be part
of the toolkit used to develop new cell types and manage increasingly complex
tasks such as nerve-gut-microbiome neuronal and hormonal communication. A
critical role of PGRMC (as one component of a new eumetazoan genetic machinery)
is proposed in LEUMCA endocrinology, neurogenesis, and nerve-gut communication
with possible involvement in circadian nicotinamide adenine dinucleotide
synthesis. This model would explain the contribution of PGRMC to metabolic and
differentiation/behavioral changes observed in age-related diseases like
diabetes, cancer and perhaps aging itself. Consistent with proposed key
regulation of neurogenesis in the LEUMCA, it is argued that Alzheimer’s disease
is the modern pathology that most closely reflects the suite of functions related
to PGRMC biology, with the ‘usual suspect’ pathologies possibly being downstream
of PGRMC1. Hopefully, these thoughts help to signpost directions for future
research.
Original language | English |
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Article number | 318 |
Number of pages | 50 |
Journal | Frontiers in Bioscience - Landmark |
Volume | 27 |
Issue number | 11 |
DOIs | |
Publication status | Published - 30 Nov 2022 |