The patent badge is an abbreviated version of the USPTO patent document. The patent badge does contain a link to the full patent document.

The patent badge is an abbreviated version of the USPTO patent document. The patent badge covers the following: Patent number, Date patent was issued, Date patent was filed, Title of the patent, Applicant, Inventor, Assignee, Attorney firm, Primary examiner, Assistant examiner, CPCs, and Abstract. The patent badge does contain a link to the full patent document (in Adobe Acrobat format, aka pdf). To download or print any patent click here.

Date of Patent:
May. 02, 2017

Filed:

Feb. 04, 2016
Applicants:

Keith R. Pennypacker, Lexington, KY (US);

Alison Willing, Tampa, FL (US);

Javier Cuevas, Lutz, FL (US);

Jon C. Antilla, Tampa, FL (US);

Michelle Cortes-salva, Fairfax, VA (US);

Inventors:

Keith R. Pennypacker, Lexington, KY (US);

Alison Willing, Tampa, FL (US);

Javier Cuevas, Lutz, FL (US);

Jon C. Antilla, Tampa, FL (US);

Michelle Cortes-Salva, Fairfax, VA (US);

Assignee:

University of South Florida, Tampa, FL (US);

Attorneys:
Primary Examiner:
Int. Cl.
CPC ...
A61K 31/155 (2006.01); C07C 279/18 (2006.01);
U.S. Cl.
CPC ...
A61K 31/155 (2013.01); C07C 279/18 (2013.01);
Abstract

A method of treating stroke by administration of a novel sigma agonist is presented. Twenty-four hours after MCAO, systemic administration of several novel sigma agonists including: Bromo-DTG; Chloro-DTG; N,N'-di-1-Naphthylguanidine hydrochloride (NAGH); N,N′-di-p-Nitrophenylguanidine HCL (NAD) or vehicle were injected subcutaneously daily for 3 days. Rats treated with Bromo-DTG and Chloro-DTG had no significant improvements in any of the motor or cognitive tests while NAGH treated rats showed improved vertical movement and had significantly less motor asymmetry and bias than vehicle treated rats. Sigma receptor agonist NAGH also was found to exert its long-term neuroprotective effects by preserving both gray matter and white matter tracts. Both NAD and NAGH, when administered 24 hours after experimental stroke, reduced neural damage and enhanced behavioral recovery thirty days later which suggests that NAGH and NAD potentially extend the therapeutic window of stroke several fold over the current treatments.


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