Age-related schwannomatosis with potential exosome-mediated contribution to prostate hyperplasia: a case report and mini-review

Author:

Chignon-Sicard Bérengère1,Hofman Véronique2,Chevallier Daniel3ORCID,Cucchi Jean-Michel4,Ilié Marius2,Dadone-Montaudié Bérengère5,Paul Florence6,Carpentier Xavier7,Quintens Hervé7,Bence-Gauchiez Coraline8,Caselles Didier9,Rossant Jacqueline10,Durand Matthieu11,Bertolotti Roger12

Affiliation:

1. Department of Plastic and Reconstructive Surgery, Pasteur 2 University Hospital, Côte d’Azur University, Nice, France

2. Laboratory of Clinical and Experimental Pathology, Pasteur 2 University Hospital, Côte d’Azur University, Nice, France

3. Department of Urology and Kidney Transplantation, Pasteur 2 University Hospital, Côte d’Azur University, 06001 Nice Cedex 1, France

4. Diagnostic Imaging Department, Princess Grace Hospital, Monaco

5. Laboratory of Solid Tumors Genetics, Nice University Hospital, Côte d’Azur University, Nice, France

6. Private Medical Imaging Center “777”, Saint-Laurent du Var, France

7. Department of Urology, Princess Grace Hospital, Monaco

8. Department of Pathology, Princess Grace Hospital, Monaco

9. Private Medical Office, Nice, France

10. Private Office of Medical Expertises, Nice, France

11. Department of Urology and Kidney Transplantation, Pasteur 2 University Hospital, Côte d’Azur University, Nice, France

12. Gene Therapy and Regulation, Faculty of Medicine, Côte d’Azur University, Nice, France

Abstract

A 72-year-old Caucasian man incurring a prostate hypertrophy presented with a right forearm nodule, the growth of which appeared to parallel the rise in his blood prostate-specific antigen (PSA) level. Echographic examination was consistent with a median-nerve schwannoma, and was confirmed upon magnetic resonance imaging (MRI). Excision of the nodule was readily performed without significant neural damage, and its schwannoma nature was confirmed upon immunohistochemistry analysis. Importantly, blood PSA dropped abruptly from ≈13 to ≈5 ng/ml within 2 months postschwannoma resection, a swift drastic reduction unachievable with oral dutasteride alone. However, 6 weeks later, a new nodule became apparent on the back of the left knee and was identified as a second schwannoma, thereby suggesting that its growth could have been stimulated by the resection of the first schwannoma, as previously described for vestibular schwannomas. The second schwannoma was in fact two: the bigger one was in the common fibular nerve and the smaller one in the tibial nerve. Both echography and MRI results were confirmed upon surgical resection of the bigger knee schwannoma. Although the third schwannoma has not yet been resected and formally characterized, we face a schwannomatosis case with an unexpected potential exosome-mediated stimulating effect on PSA secretion (PSA immunohistochemistry was negative on both schwannomas). On the other hand, preliminary genomic analysis showed a deficient balance for chromosome 22, the very chromosome carrying the three main genes involved in schwannomatosis. This age-related schwannomatosis case is thus discussed in light of the following: age-related DNA repair deficiency culminating in loss of chromosome/heterozygosity; CpG methylation/demethylation-based epigenetic aging; age-related functional decline of the immune system responsible for inefficient elimination of abnormal cells and subsequent tumorigenic cell turn-over; exosome-mediated pathologic intercellular communications; and prostate-invading brain neural progenitors as pathologic peripheral nervous system (PNS) cells.

Publisher

SAGE Publications

Subject

Urology

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