Anti-Tumor Effect against Human Cancer Xenografts by a Fully Human Monoclonal Antibody to a Variant 8-Epitope of CD44R1 Expressed on Cancer Stem Cells

Masuko, Kazue; Okazaki, Shogo; Satoh, Manabu; Tanaka, Goh; Ikeda, Tatsuya; Torii, Ryota; Ueda, Eri; Nakano, Takashi; Danbayashi, Masaaki; Tsuruoka, Tomoyo; Ohno, Yoshiya; Yagi, Hideki; Yabe, Noritsugu; Yoshida, Hiroyuki; Tahara, Tomoyuki; Kataoka, Satoshi; Oshino, Taichi; Shindo, Takayuki; Niwa, Shin Ichiro; Ishimoto, Takatsugu; Baba, Hideo; Hashimoto, Yuichi; Saya, Hideyuki; Masuko, Takashi

doi:10.1371/journal.pone.0029728

Cited by 34 publications

(18 citation statements)

References 39 publications

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“…Mazuko and collaborators demonstrated, in vivo, a protective effect of inhibiting the stem cell receptor CD44RI using an antibody against this isoform, in mice previously challenged with 1×10 6 cells from ME180, a human cervical cancer cell line [25]. Furthermore, Feng and collaborators evaluated the presence of CD44 and CK-17 in tumorigenic cervospheres injected into mice challenged with 100,000 total cervosphere cells [26].…”

Section: Discussionmentioning

confidence: 99%

Characterization of cervical cancer stem cell-like cells: phenotyping, stemness, and human papilloma virus co-receptor expression

et al. 2016

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Cancer stem cells (CSC) exhibit high tumorigenic capacity in several tumor models. We have now determined an extended phenotype for cervical cancer stem cells. Our results showed increased CK-17, p63+, AII+, CD49f+ expression in these cells, together with higher Aldehyde dehydrogenase (ALDHbright)activity in Cervical CSC (CCSC) enriched in cervospheres. An increase in stem cell markers, represented by OCT-4, Nanog, and β-catenin proteins, was also observed, indicating that under our culture conditions, CCSC are enriched in cervospheres, as compared to monolayer cultures. In addition, we were able to show that an increased ALDHbright activity correlated with higher tumorigenic activity. Flow cytometry and immunflorescence assays demonstrated that CCSC in cervosphere cultures contain a sub-population of cells that contain Annexin II, a Human papillomavirus (HPV) co-receptor. Taken together, under our conditions there is an increase in the number of CCSC in cervosphere cultures which exhibit the following phenotype: CK-17, p63+, AII+, CD49f+ and high ALDH activity, which in turn correlates with higher tumorigenicity. The presence of Annexin II and CD49f in CCSC opens the possibility that normal cervical stem cells could be the initial target of infection by high risk HPV.

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Section: Discussionmentioning

confidence: 99%

Characterization of cervical cancer stem cell-like cells: phenotyping, stemness, and human papilloma virus co-receptor expression

et al. 2016

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“…CD44 has been used for CSC detection and targeting but the mechanism of its involvement in the maintenance of CSCs is not clear. Antibodies against CD44 inhibit breast tumor growth and prevent cancer recurrence [12]. Anti-CD44 antibodies are found to induce the differentiation of acute myeloid leukemia (AML) stem cells [13].…”

Section: Introductionmentioning

confidence: 99%

Effect of CD44 Binding Peptide Conjugated to an Engineered Inert Matrix on Maintenance of Breast Cancer Stem Cells and Tumorsphere Formation

et al. 2013

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IntroductionAs cancer cells are affected by many factors in their microenvironment, a major challenge is to isolate the effect of a specific factor on cancer stem cells (CSCs) while keeping other factors unchanged. We have developed a synthetic inert 3D polyethylene glycol diacrylate (PEGDA) gel culture system as a unique tool to study the effect of microenvironmental factors on CSCs response. We have reported that CSCs formed in the inert PEGDA gel by encapsulation of breast cancer cells maintain their stemness within a certain range of gel stiffness. The objective was to investigate the effect of CD44 binding peptide (CD44BP) conjugated to the gel on the maintenance of breast CSCs.Methods4T1 or MCF7 breast cancer cells were encapsulated in PEGDA gel with CD44BP conjugation. Control groups included dissolved CD44BP and the gel with mutant CD44BP conjugation. Tumorsphere size and density, and expression of CSC markers were determined after 9 days. For in vivo, cell encapsulated gels were inoculated in syngeneic Balb/C mice and tumor formation was determined after 4 weeks. Effect of CD44BP conjugation on breast CSC maintenance was compared with integrin binding RGD peptide (IBP) and fibronectin-derived heparin binding peptide (FHBP).ResultsConjugation of CD44BP to the gel inhibited breast tumorsphere formation in vitro and in vivo. The ability of the encapsulated cells to form tumorspheres in the peptide-conjugated gels correlated with the expression of CSC markers. Tumorsphere formation in vitro was enhanced by FHBP while it was abolished by IBP.ConclusionCD44BP and IBP conjugated to the gel abolished tumorsphere formation by encapsulated 4T1 cells while FHBP enhanced tumorsphere formation compared to cells in the gel without peptide. The PEGDA hydrogel culture system provides a novel tool to investigate the individual effect of factors in the microenvironment on CSC maintenance without interference of other factors.

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“…(62) Our recent data provide evidence that the expression of CD44v and its association with an xCT CD98lc block the reactive oxygen species-induced stress signaling that results in growth arrest, cell differentiation and senescence, and, thereby, promote the proliferation of cancer cells and the formation of lethal gastrointestinal tumors, (58) and that anti-CD44v fully human mAb could inhibit tumor formation or tumor growth of xenografted human cancers. (63) Given that CD44v-expressing CSC play a central role in resistance to cancer therapy, it has been suggested that definitive treatment should target the xCT-CD44v high cell population in cancer. (58) We expect that anti-CD98 therapeutic reagents will be applied to various types of human cancers, and that CD98hc/CD98lc Fig.…”

Section: Discussionmentioning

confidence: 99%

NIH3T3 cells overexpressing CD98 heavy chain resist early G1 arrest and apoptosis induced by serum starvation

et al. 2012

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CD98 is a heterodimeric glycoprotein of 125‐kDa, which consists of a 90‐kDa heavy chain (hc) subunit and 35‐kDa to 55‐kDa light chain (lc) subunits. It is strongly expressed on the surface of proliferating normal cells and almost all tumor cells. To investigate the participation of CD98 in cellular proliferation and malignant transformation, we analyzed cell‐cycle progression of NIH3T3 clones transfected with cDNA of human CD98hc. Although NIH3T3 and control transfectant cells grown to the subconfluent state were arrested in the G0/G1 phase by serum starvation, considerable portions of CD98hc‐transfected cells resided at S and G2/M phases. Under serum‐starved and confluent conditions, significant fractions (20–25%) of NIH3T3 and control transfectant cells contained less than 2n content DNA, indicating occurrence of apoptosis, whereas no apoptotic cells were detected in CD98hc‐transfectant cells. Under serum‐starved conditions, a marked increase in the levels of cyclin D1 and cyclin E and a decrease in p16 were observed in CD98hc‐transfectant cells. The reverse was true for NIH3T3 and control transfectant cells. Our results suggest that resistance to G1 arrest and apoptosis by CD98 overexpression are associated with high G1‐cyclins and low p16 levels. (Cancer Sci, doi: 10.1111/j.1349‐7006.2012.02304.x, 2012)

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Anti-Tumor Effect against Human Cancer Xenografts by a Fully Human Monoclonal Antibody to a Variant 8-Epitope of CD44R1 Expressed on Cancer Stem Cells

Cited by 34 publications

References 39 publications

Characterization of cervical cancer stem cell-like cells: phenotyping, stemness, and human papilloma virus co-receptor expression

Characterization of cervical cancer stem cell-like cells: phenotyping, stemness, and human papilloma virus co-receptor expression

Effect of CD44 Binding Peptide Conjugated to an Engineered Inert Matrix on Maintenance of Breast Cancer Stem Cells and Tumorsphere Formation

NIH3T3 cells overexpressing CD98 heavy chain resist early G1 arrest and apoptosis induced by serum starvation

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