The Candidate Neuroprotective Agent Artemin Induces Autonomic Neural Dysplasia without Preventing Peripheral Nerve Dysfunction

Author:

Bolon Brad1,Jing Shuqian2,Asuncion Frank3,Scully Sheila1,Pisegna Marlese3,Van Gwyneth Y.1,Zheng Hu 2,Yan Bin Yu 2,Min Hosung4,Wild Ken5,Rosenfeld Robert D.6,Tarpley John1,Carnahan Josette5,Duryea Diane1,Hill Dave1,Kaufman Steve1,Yan Xiao-Qiang1,Juan Todd1,Christensen Kathy1,Mccabe James1,Simonet W. Scott7

Affiliation:

1. Departments of Pathology, Amgen Imc.

2. Department of Exploratory Biology, Amgen Imc.

3. Department of Inflammation, Amgen Imc.

4. Department of Functional Genomics, Amgen Imc.

5. Department of Neurobiology, Amgen Imc.

6. Department of Protein Chemistry, Amgen Inc., Thousand Oaks, California 91320-1799, USA

7. Department of Exploratory Biology, Amgen Imc.,

Abstract

Artemin (ART) signals through the GFR α—3/RET receptor complex to support sympathetic neuron development. Here we show that ART also influences autonomic elements in adrenal medulla and enteric and pelvic ganglia. Transgenic mice over-expressing Art throughout development exhibited systemic autonomic neural lesions including fusion of adrenal medullae with adjacent paraganglia, adrenal medullary dysplasia, and marked enlargement of sympathetic (superior cervical and sympathetic chain ganglia) and parasympathetic (enteric, pelvic) ganglia. Changes began by gestational day 12.5 and formed progressively larger masses during adulthood. Art supplementation in wild type adult mice by administering recombinant protein or an Art-bearing retroviral vector resulted in hyperplasia or neuronal metaplasia at the adrenal corticomedullary junction. Expression data revealed that Gfr α—3 is expressed during development in the adrenal medulla, sensory and autonomic ganglia and their projections, while Art is found in contiguous mesenchymal domains (especially skeleton) and in certain nerves. Intrathecal Art therapy did not reduce hypalgesia in rats following nerve ligation. These data (1) confirm that ART acts as a differentiation factor for autonomic (chiefly sympathoadrenal but also parasympathetic) neurons, (2) suggest a role for ART overexpression in the genesis of pheochromocytomas and paragangliomas, and (3) indicate that ART is not a suitable therapy for peripheral neuropathy.

Publisher

SAGE Publications

Subject

Cell Biology,Toxicology,Molecular Biology,Pathology and Forensic Medicine

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