Cellular stress induces cancer stem‐like cells through expression of <scp>DNAJB</scp>8 by activation of heat shock factor 1

Kusumoto, Hiroki; Hirohashi, Yoshihiko; Nishizawa, Satoshi; Yamashita, Masamichi; Yasuda, Kazuyo; Murai, Aiko; Takaya, Akari; Mori, Takashi; Kubo, Terufumi; Nakatsugawa, Munehide; Kanaseki, Takayuki; Tsukahara, Tomohide; Kondo, Toru; Sato, Noriyuki; Hara, Isao; Torigoe, Toshihiko

doi:10.1111/cas.13501

Cited by 21 publications

(13 citation statements)

References 37 publications

(89 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In the same study, DnaJB8 knockout in renal cell carcinoma cells conferred them sensitivity to docetaxel, thus indicating a link between HSP40 and drug resistance intrinsic to CSCs. Notably, an increase in the amounts of the SP cells and SOX2 expression was found in kidney cancer cells being subjected to heat stress; by means of DnaJB8 knockdown with siRNAs, it was shown that the observed effects were due to HSF1-induced DnaJB8 upregulation [131]. The revealed fact that both the accumulation of CSC-like cells (SP cells) and the expression of SOX2 (a transcription factor maintaining the self-renewal of CSCs [2][3][4][5]) are dependent on HSP40 and HSF1 is of importance.…”

Section: Hsp40mentioning

confidence: 99%

“…Similarly, the activating phosphorylation of HSF1 at serine 326 was shown to be critical for the maintenance of gynecologic CSCs, although the researchers explained the effect of the HSF1 activation-triggered induction of HSP27 [171]. However, not HSP27 but members of the HSP40 family, DNAJB8 [131] and DNAJA1 [134], were determined as the critical products of the heat-induced HSF1 activation/HSP expression pathway that conferred the cancer stemness-like properties. Despite some discrepancy (HSP27 vs. HSP40), HSF1 activation and subsequent expression of inducible chaperones (HSPs) in tumor cells clearly promote the CSC phenotype's acquisition.…”

Section: Hsf1 and Hsf1-activating Exposurementioning

confidence: 99%

See 1 more Smart Citation

Molecular Chaperones in Cancer Stem Cells: Determinants of Stemness and Potential Targets for Antitumor Therapy

Kabakov

Yakimova

Matchuk

2020

Cells

View full text Add to dashboard Cite

Cancer stem cells (CSCs) are a great challenge in the fight against cancer because these self-renewing tumorigenic cell fractions are thought to be responsible for metastasis dissemination and cases of tumor recurrence. In comparison with non-stem cancer cells, CSCs are known to be more resistant to chemotherapy, radiotherapy, and immunotherapy. Elucidation of mechanisms and factors that promote the emergence and existence of CSCs and their high resistance to cytotoxic treatments would help to develop effective CSC-targeting therapeutics. The present review is dedicated to the implication of molecular chaperones (protein regulators of polypeptide chain folding) in both the formation/maintenance of the CSC phenotype and cytoprotective machinery allowing CSCs to survive after drug or radiation exposure and evade immune attack. The major cellular chaperones, namely heat shock proteins (HSP90, HSP70, HSP40, HSP27), glucose-regulated proteins (GRP94, GRP78, GRP75), tumor necrosis factor receptor-associated protein 1 (TRAP1), peptidyl-prolyl isomerases, protein disulfide isomerases, calreticulin, and also a transcription heat shock factor 1 (HSF1) initiating HSP gene expression are here considered as determinants of the cancer cell stemness and potential targets for a therapeutic attack on CSCs. Various approaches and agents are discussed that may be used for inhibiting the chaperone-dependent development/manifestations of cancer cell stemness.

show abstract

Section: Hsp40mentioning

confidence: 99%

Section: Hsf1 and Hsf1-activating Exposurementioning

confidence: 99%

Molecular Chaperones in Cancer Stem Cells: Determinants of Stemness and Potential Targets for Antitumor Therapy

Kabakov

Yakimova

Matchuk

2020

Cells

View full text Add to dashboard Cite

show abstract

“…It is likely that its upregulation in tumors is in response to increased expression of many heat shock proteins, aiding tumor cell proliferation in hostile environments (16). Indeed, other HSP40 family members DNAJB6 and DNAJB8 have both been previously shown to be upregulated in cancer, contributing to cancer-initiating cell maintenance (17)(18)(19). Therapies targeting heat shock proteins and their molecular chaperones are already showing promise in cancer treatment (20).…”

Section: Discussionmentioning

confidence: 99%

Cancer Antigen Discovery Is Enabled by RNA Sequencing of Highly Purified Malignant and Nonmalignant Cells

Scurr

Greenshields‐Watson

Campbell

et al. 2020

Clinical Cancer Research

View full text Add to dashboard Cite

Broadly expressed, highly differentiated tumor-associated antigens (TAA) can elicit anti-tumor immunity. However, vaccines targeting TAAs have demonstrated disappointing clinical results, reflecting poor antigen selection and/or immunosuppressive mechanisms. Experimental design: Here, a panel of widely expressed, novel colorectal TAAs were identified by performing RNA sequencing of highly purified colorectal tumor cells in comparison to patient-matched colonic epithelial cells; tumor cell purification was essential to reveal these genes. Candidate TAA protein expression was confirmed by immunohistochemistry, and pre-existing T cell immunogenicity towards these antigens tested. Results: The most promising candidate for further development is DNAJB7 [DnaJ heat shock protein family (Hsp40) member B7], identified here as a novel cancertestis antigen. It is expressed in many tumors and is strongly immunogenic in patients with cancers originating from a variety of sites. DNAJB7-specific T cells were capable of killing colorectal tumor lines in vitro, and the IFN- + response was markedly magnified by control of immunosuppression with cyclophosphamide in cancer patients. Conclusion: This study highlights how prior methods that sequence whole tumor fractions (i.e. inclusive of alive/dead stromal cells) for antigen identification may have limitations. Through tumor cell purification and sequencing, novel candidate TAAs have been identified for future immunotherapeutic targeting.

show abstract

“…Mutations in DNAJ proteins occur frequently in neurodegenerative diseases, such as cerebellar ataxia, distal hereditary motor neuropathy and Parkinson’s disease ( Koutras & Braun, 2014 ). Nevertheless, DNAJ proteins has also been implicated in tumorogenesis and spermatogenesis ( Kusumoto et al, 2018 ; Meccariello et al, 2014 ; Nishizawa et al, 2012 ). As there are functional differences among the DNAJ proteins, it is unclear whether deficiencies in each DNAJ protein could lead to male infertility.…”

Section: Introductionmentioning

confidence: 99%

Dnajb8, a target gene of SOX30, is dispensable for male fertility in mice

Wang

Kong

et al. 2020

PeerJ

View full text Add to dashboard Cite

Background The DNAJ family of molecular chaperones maintains protein homeostasis in mitotic and postmeiotic cells, especially germ cells. Recently, we found that the transcription factor SOX30 initiates transcription of Dnajb8 during late meiosis and spermiogenesis in mouse testes. Methods We used the CRISPR/Cas9 system to generate Dnajb8 mutant mice and analyze the phenotype of the Dnajb8 mutants. Results AlthoughDnajb8 is an evolutionarily conserved gene, it is not essential for spermatogenesis and male fertility. We provide this phenotypic information, which could prevent duplicative work by other groups.

show abstract

Cellular stress induces cancer stem‐like cells through expression of DNAJB8 by activation of heat shock factor 1

Cited by 21 publications

References 37 publications

Molecular Chaperones in Cancer Stem Cells: Determinants of Stemness and Potential Targets for Antitumor Therapy

Molecular Chaperones in Cancer Stem Cells: Determinants of Stemness and Potential Targets for Antitumor Therapy

Cancer Antigen Discovery Is Enabled by RNA Sequencing of Highly Purified Malignant and Nonmalignant Cells

Dnajb8, a target gene of SOX30, is dispensable for male fertility in mice

Contact Info

Product

Resources

About