Tryptamine-Induced Tryptophanyl-tRNA^trp Deficiency in Neurodifferentiation and Neurodegeneration Interplay: Progenitor Activation with Neurite Growth Terminated in Alzheimer's Disease Neuronal Vesicularization and Fragmentation

Article type: Research Article

Authors: Paley, Elena L.^{a; b; *}

Affiliations: [a] Department of Pharmaceutical Sciences, Nova Southeastern University, Fort Lauderdale-Davie, Florida, USA | [b] Expert BioMed, Inc., Miami, FL, USA

Correspondence: [*] Correspondence to: Elena L. Paley, PhD, 1301 NE Miami Gardens Drive #302, Miami, FL 33179, USA. Tel.: +1 305 945 9080; Fax: +1 702 995 0699; E-mail: ep180@nova.edu; elena_paley@bellsouth.net.

Abstract: Tryptophanyl-tRNA synthetase (TrpRS) catalyzes tryptophanyl-tRNAtrp formation. At concentrations exceeding tryptophan, tryptamine inhibits TrpRS. This leads in tryptophanyl-tRNA deficiency and synthesis of aberrant proteins. Tryptamine presents in food and crosses blood-brain barrier. The purpose of this study is to test the hypothesis that tryptamine-induced changes in cell and animal models correlate with Alzheimer's disease (AD) manifestations. Tryptamine prevented growth of human neuroblastoma. Epithelioids recovered growth in tryptamine-free medium, while neuroblasts died. Tryptamine induced epithelioid differentiation forming synaptic vesicles, neuritic contacts, and TrpRS+ axons in stable sublines. A fraction of epithelioids was adhered to satellite cells via trypsin-resistant interdigitating junctions. Tryptamine stimulated satellite division and differentiation into neurons, transitional cell variants and neuroblasts able to repopulate. Both tryptamine-inhibited and hypoxia-downregulated TrpRS translocates into cytoplasmic extensions. TrpRS is secreted into extracellular space as a free protein or within vesicles extended from cytoplasm and then pinched-off from plasma membrane of tryptamine-treated cells. Extracellular vesicles fuse in congophilic TrpRS+ plaques in tryptamine-treated culture and AD brain. TrpRS prominent immunoreactivity is associated with plasma and vesicle membranes of satellites and AD brain degenerated neurons. Tryptamine-modified mouse brain expresses amyloid and abnormal filaments in extracellular and neuronal plasma membrane vesicles. Radiolabeled tryptamine, tryptophan and serotonin uptake was 10-fold lower in tryptamine-resistant compared to tryptamine-sensitive cells. In both variants, tryptamine uptake exceeded tryptophan uptake within 2-h assuring TrpRS inhibition. Here, tryptophanyl-tRNAtrp deficiency implicates in both neurite growth and termination/collapse. Neurite growth termination prompts TrpRS+ vesicularization. TrpRS+ vesicles contribute in neuronal fragmentation and fibrillar-vesicular congophilic plaques in AD brain.

Keywords: Alzheimer's disease, human brain, neurodifferentiation, neuronal vesicularization, progenitor, tryptamine, tryptophan, tryptophanyl-tRNA synthetase

DOI: 10.3233/JAD-2011-110176

Journal: Journal of Alzheimer's Disease, vol. 26, no. 2, pp. 263-298, 2011