PathCards: multi-source consolidation of human biological pathways

Belinky, Frida; Nativ, Noam; Stelzer, Gil; Zimmerman, Shahar; Stein, Tsippi Iny; Safran, Marilyn; Lancet, Doron

doi:10.1093/database/bav006

Cited by 227 publications

(236 citation statements)

References 45 publications

(72 reference statements)

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“…In addition, 14 of the 16 kinesins known to play critical roles in mitosis and cytokinesis in humans (36) were suppressed (Supplementary Table S1). Finally, in both MDA-MB-231 and HCC70 cells, there was a skewed JQ1-mediated downregulation of genes identified by SuperPath (37) as critical for mitosis (p<<0.001) (Fig. 3H).…”

Section: Resultsmentioning

confidence: 95%

Mitotic Vulnerability in Triple-Negative Breast Cancer Associated with LIN9 Is Targetable with BET Inhibitors

et al. 2017

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Triple-negative breast cancers (TNBC) are highly aggressive, lack FDA-approved targeted therapies, and frequently recur, making the discovery of novel therapeutic targets for this disease imperative. Our previous analysis of the molecular mechanisms of action of Bromodomain and extraterminal protein inhibitors (BETi) in TNBC revealed these drugs cause multinucleation, indicating BET proteins are essential for efficient mitosis and cytokinesis. Here, using live cell imaging, we show that BET inhibition prolonged mitotic progression and induced mitotic cell death, both of which are indicative of mitotic catastrophe. Mechanistically, the mitosis regulator LIN9 was a direct target of BET proteins that mediated the effects of BET proteins on mitosis in TNBC. While BETi have been proposed to function by dismantling super-enhancers (SE), the LIN9 gene lacks a SE but was amplified or overexpressed in the majority of TNBCs. In addition, its mRNA expression predicted poor outcome across breast cancer subtypes. Together, these results provide a mechanism for cancer selectivity of BETi that extends beyond modulation of SE-associated genes and suggest that cancers dependent upon LIN9 overexpression may be particularly vulnerable to BETi.

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Section: Resultsmentioning

confidence: 95%

Mitotic Vulnerability in Triple-Negative Breast Cancer Associated with LIN9 Is Targetable with BET Inhibitors

et al. 2017

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“…These candidate genes are either associated with cardiac channelopathies or genes of which biological function could be considered involved in SUDEP or epilepsy. This gene selection is the result of bibliographic review and online database research, including genotator [8], genecards [9], and genetest.org (which use GeneReviews and OMIM sources). In order to select the candidate genes for our study, we prioritize those genes believed to play a role in epilepsy and in sudden death.…”

Section: Custom Resequencing Panelmentioning

confidence: 99%

Genetic investigation of sudden unexpected death in epilepsy cohort by panel target resequencing

et al. 2015

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Sudden unexpected death in epilepsy (SUDEP) is defined as the abrupt, no traumatic, witnessed or unwitnessed death, occurring in benign circumstances, in an individual with epilepsy, with or without evidence for a seizure and excluding documented status epilepticus (seizure duration ≥ 30 min or seizures without recovery), and in which postmortem examination does not reveal a cause of death. Although the physiopathological mechanisms that underlie SUDEP remain to be clarified, the genetic background has been described to play a role in this disorder. Pathogenic variants in genes associated with epilepsy and encoding cardiac ion channels could explain the SUDEP phenotype. To test this we use the next-generation sequencing technology to sequence a cohort of SUDEP cases and its translation into clinical and forensic fields. A panel target resequencing was used to study 14 SUDEP cases from both postmortem (2 cases) and from living patients (12 cases). Genes already associated with SUDEP and also candidate genes had been investigated. Overall, 24 rare genetic variants were identified in 13 SUDEP cases. Four cases showed rare variants with complete segregation in the SCN1A, FBN1, HCN1, SCN4A, and EFHC1 genes, and one case with a rare variant in KCNQ1 gene showed incomplete pattern of inheritance. In four cases, rare variants were detected in CACNA1A, SCN11A and SCN10A, and KCNQ1 genes, but familial segregation was not possible due to lack of DNA from relatives. Finally, in the four remaining cases, the rare variants did not segregate in the family. This study confirms the link between epilepsy, sudden death, and cardiac disease. In addition, we identified new potential candidate genes for SUDEP: FBN1, HCN1, SCN4A, EFHC1, CACNA1A, SCN11A, and SCN10A. Further confirmation in larger cohorts will be necessary especially if genetic screening for SUDEP is applied to forensic and clinical medicine. Nevertheless, this study supports the emerging concept of a genetically determined cardiocerebral channelopathy.

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“…To make use of information from those interactomes, several integrated resources were developed, as PathCards, a systemic multisource of consolidated pathways and tools [44] or iCTNet: a Cytoscape plug-in to construct an integrative network of diseases, associated genes, drugs and tissues [45].…”

Section: Predicting Drug Response Using Network-based Approachesmentioning

confidence: 99%

Network-based approaches for drug response prediction and targeted therapy development in cancer

Dorel

Barillot

Zinovyev

et al. 2015

Biochemical and Biophysical Research Communications

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PathCards: multi-source consolidation of human biological pathways

Cited by 227 publications

References 45 publications

Mitotic Vulnerability in Triple-Negative Breast Cancer Associated with LIN9 Is Targetable with BET Inhibitors

Mitotic Vulnerability in Triple-Negative Breast Cancer Associated with LIN9 Is Targetable with BET Inhibitors

Genetic investigation of sudden unexpected death in epilepsy cohort by panel target resequencing

Network-based approaches for drug response prediction and targeted therapy development in cancer

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