cancer-stem-cells-oncology-research-2017-scientifictracks

Notes:

Volume 9, Issue 5 (Suppl)

J Cancer Sci Ther, an open access journal

ISSN: 1948-5956

Cancer Stem Cells and Oncology Research 2017

June 26-28, 2017

Page 53

International Conference on

June 26-28, 2017 London, UK

CANCER STEM CELLS AND

ONCOLOGY RESEARCH

Cancer stem cells in isocitrate dehydrogenase wild type glioblastoma express components of the renin-

angiotensin system and cathepsins B, D and G

Tinte Itinteang

, Agadha Wickremesekera

1, 2,

Helen D Brasch

, Matthew J Munro

, Paul F Davis

and

Swee T Tan

1,3

Gillies McIndoe Research Institute, Wellington, New Zealand

Wellington Regional Hospital, New Zealand

Hutt Hospital, New Zealand

Introduction

: Isocitrate dehydrogenase wildtype glioblastoma (GB), the most aggressive form of brain glioma, is associated with a

median survival of 25 months. Cancer stem cells (CSCs) have been proposed to be the origin of many cancers, including GB. Renin-

angiotensin system (RAS) has been associated in CSCs in different types of cancers. This study aimed at identifying and characterising

the CSC population within GB tissues for the CSC markers, components of the RAS, and the protease cathepsins B (CathB), D

(CathD) and G (CathG), which provide potential bypass loops for the RAS. As well neuro-spheres derived from fresh GB samples

were investigated their expression of stem cell markers, TRA 1-60, OCT4, SOX2 and SSEA-1, and the aforementioned markers.

Methodology:

DAB and immunoflourenscent immunohistochemical (IHC) staining was performed on 7 GB samples for the

expression of CSC markers SALL4, OCT4, SOX2, pSTAT3 and NANOG; components of the RAS, namely pro-renin receptor (PRR),

angiotensin converting enzyme (ACE), angiotensin II receptor 1 (ATIIR1) and angiotensin II receptor 2 (ATIIR2); and CathB, CathD

and CathG. NanoString mRNA analysis was performed on 5 of the original 7 GB samples, for the transcriptional expression of the

same markers. 6 fresh samples of the original cohort of GB were grown in culture and stained for TRA 1-60, OCT4, SSEA-1 and

SOX2, markers associated with CSCs. These cells were subjected to transcriptional analysis for CSC makers, components of RAS and

CathB, CathD and CathG.

Results:

IHC staining demonstrated a significant number of GB cells expressing SOX2 and pSTAT3. A subset of these expressedOCT4,

SALL4 and NANOG. NanoString mRNA analysis demonstrated the expression of mRNA transcripts for the markers examined.

Cultures of GB tissues yielded tumour-spheres which expressed TRA 1-60, OCT4, SSEA-1 and SOX2. These tumour-spheres also

expressed mRNA transcripts for the CSC and RAS markers, CathB and CathD demonstrated by IHC staining on GB tissues.

Conclusion:

The finding of this study confirms the putative presence of 2 CSCs within GB. The ability for primary cells derived

from GB to form tumour-spheres

in vitro

, that express CSCs markers underscores the critical role of CSCs in the biology of GB. The

expression of the components of the RAS, CathB and CathD, but not CathG by CSCs in GB and the GB-derived tumour-spheres,

suggests CSCs as a novel therapeutic target by modulation of the RAS using existing medications.

Biography

Tinte Itinteang serves as the current Chief Scientific Officer and the Evans Family Research Fellow of the Gillies McIndoe Research Institute (GMRI) in Wellington,

New Zealand. He completed his Medical Training at the Melbourne University in 2001, and then completed his Basic Medical Residency in New Zealand, from 2008-

2010. He completed his PhD from Victoria University of Wellington, NZ on the role of stem cells and the renin-angiotensin system (RAS) in infantile haemangioma.

From 2012-2014, he was appointed as a Research Fellow at the Gillies McIndoe Research Institute, during which he spent six weeks at the Friedlander laboratory

at The Scripps Research Institute in San Diego investigating the role of iPSCs for disease modelling. He was then appointed as the Chief Scientist of the GMRI

from 2015. His work on the role of stem cells and the RAS in infantile haemangioma has been acknowledged with the International Society for the Study of Vascular

Anomalies John Mulliken award as well as several national and international honours. He is the author of over 50 peer reviewed articles and has given over 100

presentations at international conferences.

tinte.itinteang@gmri.org.nz

Tinte Itinteang et al., J Cancer Sci Ther 2017, 9:5(Suppl)

DOI: 10.4172/1948-5956-C1-102