Tousled-like kinase mediated a new type of cell death pathway in Drosophila

Zhang, Y; Cai, Ruyi; Zhou, Rui; Li, Y; Liu, Lei

doi:10.1038/cdd.2015.77

Cited by 7 publications

(5 citation statements)

References 52 publications

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“…This is in line with previous data, where TLK1 overexpression in breast and prostate cancer resulted in resistance to radiotherapy (52). By contrast, Zhang et al (53) observed that TLK1 overexpression in Drosophila eyes induced cell death and pigmentation loss, suggesting that TLK1 may serve a different role in eye development.…”

Section: Identification Of Novel Targets By Integration Of In Silico supporting

confidence: 92%

Knockdown of Tousled‑like kinase 1 inhibits survival of glioblastoma multiforme cells

et al. 2020

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Glioblastoma multiforme (GBM) is an aggressive type of brain tumour that commonly exhibits resistance to treatment. The tumour is highly heterogenous and complex kinomic alterations have been reported leading to dysregulation of signalling pathways. The present study aimed to investigate the novel kinome pathways and to identify potential therapeutic targets in GBM. Meta-analysis using Oncomine identified 113 upregulated kinases in GBM. RNAi screening was performed on identified kinases using ON-TARGETplus siRNA library on LN18 and U87MG. Tousled-like kinase 1 (TLK1), which is a serine/threonine kinase was identified as a potential hit. In vitro functional validation was performed as the role of TLK1 in GBM is unknown. TLK1 knockdown in GBM cells significantly decreased cell viability, clonogenicity, proliferation and induced apoptosis. TLK1 knockdown also chemosensitised the GBM cells to the sublethal dose of temozolomide. The downstream pathways of TLK1 were examined using microarray analysis, which identified the involvement of dNA replication, cell cycle and focal adhesion signalling pathways. In vivo validation of the subcutaneous xenografts of stably transfected sh-TLK1 U87MG cells demonstrated significantly decreased tumour growth in female BALB/c nude mice. Together, these results suggested that TLK1 may serve a role in GBM survival and may serve as a potential target for glioma.

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Section: Identification Of Novel Targets By Integration Of In Silico supporting

confidence: 92%

Knockdown of Tousled‑like kinase 1 inhibits survival of glioblastoma multiforme cells

et al. 2020

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“…This differs from the severe rough-eye phenotype caused by Tak1 overexpression alone, in which JNK activity is activated and induces apoptosis 41 . Although Tlk overexpression induces cell death, the regulatory pathway is not through apoptosis 42 . Thus, the difference may result from alternative functions of Tak1 when it works with different partners.…”

Section: Discussionmentioning

confidence: 99%

Inactive Tlk associating with Tak1 increases p38 MAPK activity to prolong the G2 phase

Liaw¹,

Chiang

2019

Sci Rep

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To guard genome integrity, response mechanisms coordinately execute the G2/M checkpoint in responding to stress. p38 MAPK is activated to prolong the G2 phase for completion of damage repair. Tlk activity is required for DNA repair, chromosome segregation and G2 recovery. However, the involvement of Tlk in G2 recovery differs from previous findings that Tlk overexpression delays the G2/M transition. To clarify this difference, genetic interaction experiments were performed using the second mitotic wave as model system. The results indicate that Tlk overexpression prolongs the G2 phase through p38 MAPK activation, independent of Tlk kinase activity. The results of co-immunoprecipitation, database search and RNAi screening suggest that eEF1α1 and Hsc70-5 links Tlk to Tak1. Reduced gene activities of Tlk, Hsc70-5, eEF1α1 and/or Tak1 couldn’t prolong the G2 phase induced by heat shock, indicating that these proteins work together to elevate p38 MAPK activity. In contrast, a high level of wild type Tlk decreases phosphorylated p38 MAPK levels. Thus, the difference is explained by a dual function of Tlk. When under stress, inactive Tlk increases p38 MAPK activity to prolong the G2 phase, and then activated Tlk modulates activities of p38 MAPK and Asf1 to promote G2 recovery afterwards.

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“…By this genetic screening, we identified 14 genes whose mutation or knockdown effectively suppressed the rough eye phenotype induced by caz knockdown, whereas there were 5 genes whose mutation or knockdown strongly enhanced the rough eye phenotype (to be published elsewhere). The 14 suppressor genes included Histone acetyltransferase 1 (Hat1) [ 120 , 121 ], chameau ( chm ) [ 122 , 123 ], N(alpha)-acetyltransferase 60 (Naa60) [ 124 ], Negative Cofactor 2β (Nc2β) [ 125 ], Spt7 [ 126 ], TBP-associated factor 1(Taf1) [ 127 ], will die slowly (wds) [ 125 ], Sirtuin 2 (Sirt2) [ 128 ], Methyltransferase 2(Mt2) [ 129 ], extra sexcombs (esc) [ 130 ], grappa (gpp) [ 131 ], SET domain containing 1 (Set1) [ 132 ], Tousled-like kinase (Tlk) [ 133 ], and Vacuolar protein sorting 11(Vps11) [ 134 ]. Among them, mutations of chm and Naa60 suppressed the locomotive defects and morphological defects of synapse at the NMJ induced by caz knockdown (to be published elsewhere).…”

Section: Epigenetic Regulation Of Alsmentioning

confidence: 99%

Epigenetic Regulation of ALS and CMT: A Lesson from Drosophila Models

Yamaguchi

Omori

Asada

et al. 2021

IJMS

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Amyotrophic lateral sclerosis (ALS) is the third most common neurodegenerative disorder and is sometimes associated with frontotemporal dementia. Charcot–Marie–Tooth disease (CMT) is one of the most commonly inherited peripheral neuropathies causing the slow progression of sensory and distal muscle defects. Of note, the severity and progression of CMT symptoms markedly vary. The phenotypic heterogeneity of ALS and CMT suggests the existence of modifiers that determine disease characteristics. Epigenetic regulation of biological functions via gene expression without alterations in the DNA sequence may be an important factor. The methylation of DNA, noncoding RNA, and post-translational modification of histones are the major epigenetic mechanisms. Currently, Drosophila is emerging as a useful ALS and CMT model. In this review, we summarize recent studies linking ALS and CMT to epigenetic regulation with a strong emphasis on approaches using Drosophila models.

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Tousled-like kinase mediated a new type of cell death pathway in Drosophila

Cited by 7 publications

References 52 publications

Knockdown of Tousled‑like kinase 1 inhibits survival of glioblastoma multiforme cells

Knockdown of Tousled‑like kinase 1 inhibits survival of glioblastoma multiforme cells

Inactive Tlk associating with Tak1 increases p38 MAPK activity to prolong the G2 phase

Epigenetic Regulation of ALS and CMT: A Lesson from Drosophila Models

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