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Gastric cancer (GC) is the third and fifth cause of cancer‐associated mortality for men and women throughout the world, respectively. Despite the use of surgery and chemotherapy for GC therapy, there are no efficient therapeutic protocols for it to ...
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RISS 인기검색어
Isolation and identification of chemotherapy‐enriched sphere‐forming cells from a patient with gastric cancer
한글로보기https://www.riss.kr/link?id=O119383050
- 저자
- 발행기관
- 학술지명
- 권호사항
-
발행연도
2018년
-
작성언어
-
-
Print ISSN
0021-9541
-
Online ISSN
1097-4652
-
등재정보
SCI;SCIE;SCOPUS
-
자료형태
학술저널
-
수록면
7036-7046 [※수록면이 p5 이하이면, Review, Columns, Editor's Note, Abstract 등일 경우가 있습니다.]
- 소장기관
-
구독기관
- 전북대학교 중앙도서관
- 성균관대학교 중앙학술정보관
- 부산대학교 중앙도서관
- 전남대학교 중앙도서관
- 제주대학교 중앙도서관
- 중앙대학교 서울캠퍼스 중앙도서관
- 인천대학교 학산도서관
- 숙명여자대학교 중앙도서관
- 서강대학교 로욜라중앙도서관
- 계명대학교 동산도서관
- 충남대학교 중앙도서관
- 한양대학교 백남학술정보관
- 이화여자대학교 중앙도서관
- 고려대학교 도서관
-
0
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부가정보
다국어 초록 (Multilingual Abstract)
Gastric cancer (GC) is the third and fifth cause of cancer‐associated mortality for men and women throughout the world, respectively. Despite the use of surgery and chemotherapy for GC therapy, there are no efficient therapeutic protocols for it to date. Cancer stem cells (CSCs) due to their pivotal role in tumor initiation, growth, progression, invasion, distant metastasis, recurrence and resistance to anticancer drugs are very appealing targets for cancer therapies. Here, we isolated and identified CSCs from a chemotherapy‐treated patient. Small subpopulation of dissociated cells after tissue digestion formed spheroid colonies in serum‐free media under the non‐adherent condition. These spheroid colonies differentiated into epithelial like cells in serum‐containing medium. Few sphere‐forming cells carried CD44 and CD54 markers overexpressed DLL4 that is responsible for tumor growth and angiogenesis. Subcutaneous injections of sphere‐forming cells in different passages conferred tumorigenicity in nude mice. Sphere‐forming cells upregulated CD44 polymorphisms CD44v3, ‐v6, and ‐v8 ‐10, stemness factors OCT4, SOX2, SALL4 and Cripto‐1, self‐renewal molecules IHh, Wnt, β‐catenin and BMI1, and epithelial mesenchymal transition (EMT) markers Twist1 and Snail1 in vitro and in vivo. Moreover, these cells similar to sphere‐forming cells isolated from a chemotherapy‐free patient expressed Oct‐4 and β‐catenin proteins. However, the Twist1 protein was only expressed by sphere‐forming cells derived from the chemotherapy‐treated patient. Thus, these cells have all the characteristics of stationary and migratory CSCs, including tumorigenicity, self‐renewal, pluripotency, invasion and metastasis. Taken together, targeting chemotherapy‐enriched CSCs as chemo‐resistance cells observed in GC patients can provide more effective therapeutic strategies compared to untreated patients.
Sphere‐forming cells derived from a chemotherapy‐treated patient were enriched in tumor mass. These cells have all the characteristics of stationary and migratory CSCs, including tumorigenicity, self‐renewal, pluripotency, invasion and metastasis. Targeting chemotherapy‐enriched CSCs can provide effective therapeutic strategies.
Sphere‐forming cells derived from a chemotherapy‐treated patient were enriched in tumor mass. These cells have all the characteristics of stationary and migratory CSCs, including tumorigenicity, self‐renewal, pluripotency, invasion and metastasis. Targeting chemotherapy‐enriched CSCs can provide effective therapeutic strategies.
Gastric cancer (GC) is the third and fifth cause of cancer‐associated mortality for men and women throughout the world, respectively. Despite the use of surgery and chemotherapy for GC therapy, there are no efficient therapeutic protocols for it to date. Cancer stem cells (CSCs) due to their pivotal role in tumor initiation, growth, progression, invasion, distant metastasis, recurrence and resistance to anticancer drugs are very appealing targets for cancer therapies. Here, we isolated and identified CSCs from a chemotherapy‐treated patient. Small subpopulation of dissociated cells after tissue digestion formed spheroid colonies in serum‐free media under the non‐adherent condition. These spheroid colonies differentiated into epithelial like cells in serum‐containing medium. Few sphere‐forming cells carried CD44 and CD54 markers overexpressed DLL4 that is responsible for tumor growth and angiogenesis. Subcutaneous injections of sphere‐forming cells in different passages conferred tumorigenicity in nude mice. Sphere‐forming cells upregulated CD44 polymorphisms CD44v3, ‐v6, and ‐v8 ‐10, stemness factors OCT4, SOX2, SALL4 and Cripto‐1, self‐renewal molecules IHh, Wnt, β‐catenin and BMI1, and epithelial mesenchymal transition (EMT) markers Twist1 and Snail1 in vitro and in vivo. Moreover, these cells similar to sphere‐forming cells isolated from a chemotherapy‐free patient expressed Oct‐4 and β‐catenin proteins. However, the Twist1 protein was only expressed by sphere‐forming cells derived from the chemotherapy‐treated patient. Thus, these cells have all the characteristics of stationary and migratory CSCs, including tumorigenicity, self‐renewal, pluripotency, invasion and metastasis. Taken together, targeting chemotherapy‐enriched CSCs as chemo‐resistance cells observed in GC patients can provide more effective therapeutic strategies compared to untreated patients.
Sphere‐forming cells derived from a chemotherapy‐treated patient were enriched in tumor mass. These cells have all the characteristics of stationary and migratory CSCs, including tumorigenicity, self‐renewal, pluripotency, invasion and metastasis. Targeting chemotherapy‐enriched CSCs can provide effective therapeutic strategies.
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