ERBB3: A potential serum biomarker for early detection and therapeutic target for devil facial tumour 1 (DFT1)

Hayes, Dane; Kunde, Dale; Taylor, Rennae S.; Pyecroft, Stephen; Sohal, Sukhwinder Singh; Snow, Elizabeth T.

doi:10.1371/journal.pone.0177919

Cited by 8 publications

(10 citation statements)

References 205 publications

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“…Interestingly, both PDGFA and PDGFB , encoding ligands for PDGFRs, have undergone copy number gains in DFT1 (and PDGFA is additionally involved in a SV in DFT1 [ Murchison et al., 2012 ; Tables S4 and S5 ]). Furthermore, ERBB3 showed copy number gains in DFT1 and is expressed in DFT1 ( Hayes et al., 2017 , Taylor et al., 2017 ), and a subset of DFT1s carried gains of NRG2 , encoding an ERBB ligand ( Figure 4 B; Tables S3 and S4 ).…”

Section: Resultsmentioning

confidence: 99%

“…Tissues were orientated on the EG1160 (Leica Microsystems), embedded in paraffin wax (Leica Microsystems) and sectioned at 3 microns using a Leica RM2245 microtome and adhered to microscope slides (Menzel Gläser, Thermo Fisher Scientific) for 20 min at 60°C. Sections were deparaffinized, rehydrated and stained using Jung autostainer XL (Leica Microsystems) for Hematoxylin (Australian Biostain) and Eosin, dehydrated, cleared, cover slipped (Leica Microsystems) and mounted in CV Mount (Leica Microsystems) ( Hayes et al., 2017 ).…”

Section: Methodsmentioning

confidence: 99%

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The Origins and Vulnerabilities of Two Transmissible Cancers in Tasmanian Devils

et al. 2018

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SummaryTransmissible cancers are clonal lineages that spread through populations via contagious cancer cells. Although rare in nature, two facial tumor clones affect Tasmanian devils. Here we perform comparative genetic and functional characterization of these lineages. The two cancers have similar patterns of mutation and show no evidence of exposure to exogenous mutagens or viruses. Genes encoding PDGF receptors have copy number gains and are present on extrachromosomal double minutes. Drug screening indicates causative roles for receptor tyrosine kinases and sensitivity to inhibitors of DNA repair. Y chromosome loss from a male clone infecting a female host suggests immunoediting. These results imply that Tasmanian devils may have inherent susceptibility to transmissible cancers and present a suite of therapeutic compounds for use in conservation.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

The Origins and Vulnerabilities of Two Transmissible Cancers in Tasmanian Devils

et al. 2018

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“…The underlying mechanism of maintained STAT3 activation and the apparent lack of negative regulation requires further investigation. Mutually not exclusive, the involved processes may include recently detected copy gains of ERBB3 (Hayes et al, 2017; Taylor et al, 2017) leading to enhanced ERBB2-ERBB3 heterodimer activity, the secretion of ligands of the ERBB family, blunted negative control by phosphatases or the SOCS-ubiquitin pathway ( Fig. S5 ).…”

Section: Discussionmentioning

confidence: 99%

The ERBB-STAT3 Axis Drives Tasmanian Devil Facial Tumor Disease

Kosack

Wingelhofer

Popa

et al. 2018

Preprint

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1The marsupial Tasmanian devil (Sarcophilus harrisii) faces extinction due to transmissible devil 2 facial tumor disease (DFTD). To unveil the molecular underpinnings of DFTD, we designed an 3 approach that combines sensitivity to drugs with an integrated systems-biology characterization. 4 Sensitivity to inhibitors of the ERBB family of receptor tyrosine kinases correlated with their 5 overexpression, suggesting a causative link. Proteomic and DNA methylation analyses revealed 6 tumor-specific signatures linked to oncogenic signaling hubs including evolutionary conserved 7 STAT3. Indeed, ERBB inhibition blocked phosphorylation of STAT3 and arrested cancer cells. 8 Pharmacological blockade of ERBB signaling prevented tumor growth in a xenograft model and 9 resulted in recovery of MHC class I gene expression. This link between the hyperactive ERBB-10

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“…NF2, ErbB3 and downstream effectors PI3K-Akt or MAPK signalling pathways are therefore prime candidates for future immunohistochemistry and functional studies to determine if they are involved in DFT1 tumourigenesis. It has recently been shown that elevated levels of ErbB3 are detectable in devil sera several months prior to visual tumour eruptions 34 making it imperative that the pathway involving NF2 and ErbB3 be prioritised for further investigation. Additionally, germline mutations in the tumour suppressor LZTR1 are associated with a predisposition for an inherited disorder responsible for the development of multiple schwannomas in humans 35 , making the entire NF2 region a high priority for further investigation.…”

Section: Discussionmentioning

confidence: 99%

Identification of candidate genes for devil facial tumour disease tumourigenesis

Taylor

Zhang

Schöning

et al. 2017

Sci Rep

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Devil facial tumour (DFT) disease, a transmissible cancer where the infectious agent is the tumour itself, has caused a dramatic decrease in Tasmanian devil numbers in the wild. The purpose of this study was to take a candidate gene/pathway approach to identify potentially perturbed genes or pathways in DFT. A fusion of chromosome 1 and X is posited as the initial event leading to the development of DFT, with the rearranged chromosome 1 material now stably maintained as the tumour spreads through the population. This hypothesis makes chromosome 1 a prime chromosome on which to search for mutations involved in tumourigenesis. As DFT1 has a Schwann cell origin, we selected genes commonly implicated in tumour pathways in human nerve cancers, or cancers more generally, to determine whether they were rearranged in DFT1, and mapped them using molecular cytogenetics. Many cancer-related genes were rearranged, such as the region containing the tumour suppressor NF2 and a copy gain for ERBB3, a member of the epidermal growth factor receptor family of receptor tyrosine kinases implicated in proliferation and invasion of tumours in humans. Our mapping results have provided strong candidates not previously detected by sequencing DFT1 genomes.

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ERBB3: A potential serum biomarker for early detection and therapeutic target for devil facial tumour 1 (DFT1)

Cited by 8 publications

References 205 publications

The Origins and Vulnerabilities of Two Transmissible Cancers in Tasmanian Devils

The Origins and Vulnerabilities of Two Transmissible Cancers in Tasmanian Devils

The ERBB-STAT3 Axis Drives Tasmanian Devil Facial Tumor Disease

Identification of candidate genes for devil facial tumour disease tumourigenesis

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