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Query: EC:2.7.10.1 (
ERK
)
95,504
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Next-generation sequencing of cell-free circulating DNA (cfDNA) has emerged as promising technique for identifying minimally invasive genomic profiling of tumor cells recently. However, it remains relatively unknown in
LAM
disease. In our study, paired cfDNA and genomic DNA (gDNA) in blood samples were obtained from 23
LAM
patients and seven healthy controls to explore mutations profiles of targeted 70 cancer-related genes. As results, log2-based allele frequencies of mutations in cfDNA were significantly different from those of gDNA. By comparing the mutual mutations identified both in cfDNA and gDNA, a significant correlation was also observed. After removing mutations in gDNA, distinct somatic mutation profiles of cfDNA were observed in
LAM
patients. Forty of 70 targeted genes had recurrent mutations, of which ATM, BRCA2 and APC showed the highest frequency. Based on the mutation, correlation network constructed of 40 mutated genes, 11 hub genes bearing intensive interactions were highlighted, including BRCA1, BRCA2, RAD50, RB1, NF1, APC, MLH3, ATM,
PDGFRA
, PALB2 and BLM. Expression of the hub genes showed significant clusters between
LAM
patients and controls and that RAD50 and BRCA2 had the strongest associations with subject phenotypes. Myogenesis and estrogen response were confirmed to be positively regulated in
LAM
patients. Collectively, our study provided a landscape of genomic alterations in
LAM
and discovered several potential driver genes, that is, BRCA2 and RAD50, which shed a substantial light on the clinical application of key molecular markers and potential therapy targets for precision diagnosis and treatment in the future.
...
PMID:Identification of driver genes and somatic mutations in cell-free DNA of patients with pulmonary lymphangioleiomyomatosis. 3119 8
Acute myeloid leukemias (AML) harboring a constitutively active internal tandem duplication (ITD) mutation in the
FMS
-like kinase tyrosine kinase (
FLT3
) receptor are associated with poor patient prognosis. Despite initial clinical responses to
FLT3
kinase inhibitors, patients eventually relapse. Mechanisms of resistance include the acquisition of secondary
FLT3
mutations and protective stromal signaling within the bone marrow niche. Here we show that
LAM
-003, a prodrug of the heat shock protein 90 inhibitor
LAM
-003A, has cytotoxic activity against AML cell lines and primary samples harboring
FLT3
-ITD.
LAM
-003 regressed tumors in an MV-4-11 xenograft mouse model and extended survival in a MOLM-13 systemic model.
LAM
-003 displayed synergistic activity with chemotherapeutic drugs and
FLT3
inhibitors, with the most robust synergy being obtained with venetoclax, a BCL-2 inhibitor. This finding was verified in a MOLM-13 systemic survival model in which the combination significantly prolonged survival compared with the single agents. Importantly,
LAM
-003 exhibited equipotent activity against
FLT3
inhibitor-resistant mutants of
FLT3
, such as D835 or F691, in cytotoxic and
FLT3
degradation assays.
LAM
-003 also retained potency in AML cells grown in stromal-conditioned media that were resistant to
FLT3
inhibitors. Lastly, a genome-wide CRISPR screen revealed epigenetic regulators, including KDM6A, as determinants of
LAM
-003 sensitivity in AML cell lines, leading to the discovery of synergy with an EZH2 inhibitor. Collectively, these preclinical findings support the use of
LAM
-003 in
FLT3
-ITD patients with AML who no longer respond to
FLT3
inhibitor therapy either as a single agent or in combination with drugs known to be active in AML.
...
PMID:LAM-003, a new drug for treatment of tyrosine kinase inhibitor-resistant FLT3-ITD-positive AML. 3175 72
We previously reported the benefit of lomustine addition to conventional chemotherapy in older acute myeloid leukemias with nonadverse chromosomal aberrations in the
LAM
-SA 2007 randomized clinical trial (NCT00590837). A molecular analysis of 52 genes performed in 330 patients included in this trial, 163 patients being treated with lomustine in combination with idarubicin and cytarabine and 167 without lomustine, identified 1088 mutations with an average of 3.3 mutations per patient. NPM1,
FLT3
, and DNMT3A were the most frequently mutated genes. A putative therapeutic target was identified in 178 patients (54%). Among five molecular classifications analyzed, the ELN2017 risk classification has the stronger association with the clinical evolution. Patients not treated with lomustine have an expected survival prognosis in agreement with this classification regarding the overall and event-free survivals. In strong contrast, lomustine erased the ELN2017 classification prognosis. The benefit of lomustine in nonadverse chromosomal aberrations was restricted to patients with RUNX1, ASXL1, TP53, and
FLT3
-ITD
high
/NPM1
WT
mutations in contrast to the intermediate and favorable ELN2017 patients. This post-hoc analysis identified a subgroup of fit elderly AML patients with intermediate cytogenetics and molecular markers who may benefit from lomustine addition to intensive chemotherapy.
...
PMID:Lomustine is beneficial to older AML with ELN2017 adverse risk profile and intermediate karyotype: a FILO study. 3294 50
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