Claudin7-dependent exosome-promoted reprogramming of nonmetastasizing tumor cells.

Kyuno, Daisuke; Zhao, Kun; Zöller, Margot; Provaznik, Jan; Hackert, Thilo; Schnölzer, Martina

doi:10.1002/ijc.32312

Journal Article

DKFZ-2019-01377

Claudin7-dependent exosome-promoted reprogramming of nonmetastasizing tumor cells.

Kyuno, D. ; Zhao, K. ; Schnölzer, M.DKFZ* ; Provaznik, J. ; Hackert, T. ; Zöller, M.

2019
Wiley-Liss Bognor Regis

International journal of cancer 145(8), 2182-2200 (2019) [10.1002/ijc.32312]

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Please use a persistent id in citations: doi:10.1002/ijc.32312

Abstract: Claudin7 (cld7) is a cancer-initiating cell (CIC) marker in gastrointestinal tumors, a cld7-knockdown (kd) being accompanied by loss of tumor progression. Tumor exosomes (TEX) restoring CIC activities, we explored the contribution of cld7. This became particularly interesting, as tight junction (TJ)- and glycolipid-enriched membrane domain (GEM)-derived cld7 is recruited into distinct TEX. TEXs were derived from CIC or cld7kd cells of a rat pancreatic and a human colon cancer line. TEX derived from pancreatic cancer cld7kd cells rescued with palmitoylation site-deficient cld7 (cld7mP) allowed selectively evaluating the contribution of GEM-derived TEX, only palmitoylated cld7 being integrated into GEM. Cld7 CIC-TEX promoted tumor cell dissemination and metastatic growth without a major impact on proliferation, apoptosis resistance and epithelial-mesenchymal transition. Instead, migration, invasion and (lymph)angiogenesis were strongly supported, only migration being selectively fostered by GEM-derived cld7 TEX. CIC-TEX coculture of cld7kd cells uncovered significant changes in the cld7kd cell protein and miRNA profiles. However, changes did not correspond to the CIC-TEX profile, CIC-TEX rather initiating integrin, protease and RTK, particularly lymphangiogenic receptor activation. CIC-TEX preferentially rescuing cld7kd-associated defects in signal transduction was backed up by an RTK inhibitor neutralizing the impact of CIC-TEX on tumor progression. In conclusion, cld7 contributes to selective steps of the metastatic cascade. Defects of cld7kd and cld7mP cells in migration, invasion and (lymph)angiogenesis are effaced by CIC-TEX that act by signaling cascade activation. Accordingly, RTK inhibitors are an efficient therapeutic defeating CIC-TEX.

Classification:

ddc:610

Contributing Institute(s):

Funktionelle Proteomanalyse (B100)

Research Program(s):

312 - Functional and structural genomics (POF3-312) (POF3-312)

Appears in the scientific report 2019

Database coverage:
Medline

; BIOSIS Previews ; Clarivate Analytics Master Journal List ; Current Contents - Life Sciences ; IF >= 5 ; JCR ; NCBI Molecular Biology Database ; Nationallizenz

; SCOPUS ; Science Citation Index ; Science Citation Index Expanded ; Web of Science Core Collection

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Record created 2019-06-04, last modified 2024-02-29

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