T cell leukemia control via Ras-Raf pathway inhibition with peptides • JML Journal of Medicine and Life

2017, Volume 10, Issue 3, pp 172 – 175

T cell leukemia control via Ras-Raf pathway inhibition with peptides

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Authors and Affiliations

Marin G ^*

Bruzzoni-Giovanelli H ^**

Schinella G ^***

* *National University of La Plata - CONICET, Pharmacology Rebollo, Angelita; CIMI, Inserm/UPMC/CNRS- Université Pierre et Marie Curie, Paris 6, France; Centre d’Immunologie et des Maladies Infectieuses Piazzon, Isabel; National Academia of Medicine, Argentina, Immunology Researcher of the Experimental Immunology Laboratory

** **Université Paris 7- Hôpital Saint Louis, Pharmacology - Centre d’Investigations Cliniques Duarte, Alejandra; National Academia of Medicine, Experimental Immunology Laboratory

*** ***National University of La Plata, Pharmacology Errecalde, Jorge; Universidad Nacional de la Plata Facultad de Ciencias Medicas

Correspondence to: Gustavo H. Marin, MD, PhD, National University of Medicine La Plata, CONICET, Argentina Research Group Sorbonne Paris Cite - CIN 60 y 120, Code 1900, La Plata, Argentina, Mobile phone: +5492215030058, E-mail: gmarin2009@gmail.com

Abstract

RATIONALE: RAS-RAF-MEK-ERK pathway has been considered a promising target for anticancer therapy. However, tumor cells may develop resistance against such drugs via hyperactivation of N-Ras, which explains why novel therapeut-ic approaches. In this sense, the Institute Curie- Université Pierre et Marie Curie (Paris 6) designed peptides in order to disturb Ras/Raf interaction which showed pro-apoptotic properties. These peptides were patented as WO2015001045 A2 (PCT/EP2014/064243)5.

OBJECTIVE: In order to check the anti-tumoral action of WO2015001045 A2 peptides in a very aggressive BALB/c mice spontaneous leukemia called LB, we performed the present study.

METHOD & RESULTS: 50 BALB/c mice inoculated with 106 LB tumor cells were randomly assigned either to control (placebo) or treatment group (that daily received 3 mg of peptide per kg of mice) during 30 days. By day 15 only 24% of the control group was alive vs. 100% of the treatment group. The average survival in treated group was 20,27 days while in control group the mean survival was 15,48 days. Either bone marrow, spleen or axillary nodes demonstrated a higher level of malignant T cell presence compare with treated group (89,78% ; 95,64% & 77,68% versus 72,45%, 80,23% & 63.44% respectively for each organ inspected.

DISCUSSION: Our study demonstrated an improvement in survival curves in mice model affected by spontaneous T lymphoid leukemia when peptides WO2015001045 A2 were used. These peptides might be a valid option to become part of the therapeutic armory for malignant lymphoproliferative diseases control.

Keywords

peptidescancerleukemiacontrolmice

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About this article

PMC ID: 5652266
PubMed ID: 29075346
DOI:

Article Publishing Date (print): Jul-Sep 2017
Available Online:

Journal information

ISSN Printing: 1844-122X
ISSN Online: 1844-3117
Journal Title: Journal of Medicine and Life

Copyright License: Open Access

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