Tumor-initiating Cells Are Rare in Many Human Tumors

Overview

Journal Cell Stem Cell

Publisher Cell Press

Specialty Cell Biology

Date 2010 Sep 1

PMID 20804964

Citations 127

Authors

Kota Ishizawa

Zeshaan A Rasheed

Robert Karisch

Qiuju Wang

Jeanne Kowalski

Erica Susky

Keira Pereira

Christina Karamboulas

Nadeem Moghal

N V Rajeshkumar

Manuel Hidalgo

Ming Tsao

Laurie Ailles

Thomas K Waddell

Anirban Maitra

Benjamin G Neel

William Matsui

Affiliations

Soon will be listed here.

Abstract

Tumor-initiating cells (TICs) are defined by their ability to form tumors after xenotransplantation in immunodeficient mice and appear to be relatively rare in most human cancers. Recent data in melanoma indicate that the frequency of TICs increases dramatically via more permissive xenotransplantation conditions, raising the possibility that the true frequency of TICs has been greatly underestimated in most human tumors. We compared the growth of human pancreatic, non-small cell lung, and head and neck carcinomas in NOD/SCID and NSG mice. Although TIC frequency was detected up to 10-fold higher in NSG mice, it remained low (<1 in 2500 cells) in all cases. Moreover, aldehyde dehydrogenase-positive (ALDH(+)) and CD44(+)CD24(+) cells, phenotypically distinct cells enriched in TICs, were equally tumorigenic in NOD/SCID and NSG mice. Our findings demonstrate that TICs are rare in these cancers and that the identification of TICs and their frequency in other human malignancies should be validated via primary tumors and highly permissive xenotransplantation conditions.

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