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BIOMARKER:

KIT N822K

i
Other names: KIT, C-Kit, CD117, PBT, SCFR, Stem Cell Factor Receptor, V-kit Hardy-Zuckerman 4 feline sarcoma viral oncogene homolog
Entrez ID:
9ms
Usefulness of KIT mutant transcript levels for monitoring measurable residual disease in t (8;21) acute myeloid leukemia. (PubMed, Hematol Oncol)
After Course 2 consolidation, the KIT_H patients with >3-log reduction in the RUNX1::RUNX1T1 transcript levels (11/45; 24.4%) had similar RFS as that of patients with <3-log reduction in the RUNX1::RUNX1T1 transcript levels. The combination of KITmut and RUNX1::RUNX1T1 transcript levels after Course 2 consolidation may improve risk stratification in t (8; 21) AML patient with KIT mutation.
Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase) • RUNX1 (RUNX Family Transcription Factor 1) • RUNX1T1 (RUNX1 Partner Transcriptional Co-Repressor 1)
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KIT mutation • KIT N822K • KIT D816V
1year
Analysis of Safety and Efficacy of Avapritinib As Targeted Therapy for Pediatric Acute Myeloid Leukemia Patients with KIT Mutation after Transplantation (ASH 2023)
2 patients did not achieve continuous RUNX1: : RUNX1T1 negative after preemptive therapy with Decitabine (DAC) and donor lymph infusion (DLI), and then was treated with Avapritinib, one's RUNX1: : RUNX1T1 fusion achieved continuously negative after 1 month treatment of Avapritinib, the other's achieved continuous negative after 7 months treatment of Avapritinib. Avapritinib is safe and effective in the prophylactic and preemptive treatment of AML with KIT mutation after allo-HSCT in children, which provides a clinical drug for the prevention of relapse after transplantation.
Clinical
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KIT (KIT proto-oncogene, receptor tyrosine kinase) • RUNX1 (RUNX Family Transcription Factor 1) • RUNX1T1 (RUNX1 Partner Transcriptional Co-Repressor 1)
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KIT mutation • RUNX1 mutation • KIT N822K • KIT exon 17 mutation • RUNX1-RUNX1T1 fusion • KIT fusion
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decitabine • Ayvakit (avapritinib)
1year
RASMULTI(ON) Inhibitor RMC-7977 Targets Oncogenic RAS Mutations and Overcomes RAS/MAPK-Mediated Resistance to FLT3 Inhibitors in AML Models (ASH 2023)
RMC-7977 is a potent, oral small molecule inhibitor of both wild-type and mutant GTP-bound RAS oncoproteins (RASMULTI) and is a preclinical tool compound representative of the clinical candidate RMC-6236, currently in clinical evaluation (NCT05379985)...Gilteritinib and the gilteritinib/venetoclax combination selected for survival of cells harboring NRAS mutations, but RMC-7977 inhibited outgrowth of all cell populations...In vivo studies investigating the tolerability and activity of RMC-7977 and RMC-7977 combinations in RAS mutant/FLT3i-resistant patient-derived xenograft models are ongoing and will be presented. Collectively, our data provide preclinical evidence that combination therapies leveraging RASMULTI(ON) inhibition are effective in suppressing RAS-mutant AML clones, a common mechanism of resistance to currently approved targeted therapies in AML and a current area of high unmet clinical need.
IO biomarker
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KRAS (KRAS proto-oncogene GTPase) • FLT3 (Fms-related tyrosine kinase 3) • NRAS (Neuroblastoma RAS viral oncogene homolog) • KIT (KIT proto-oncogene, receptor tyrosine kinase) • IDH1 (Isocitrate dehydrogenase (NADP(+)) 1) • IDH2 (Isocitrate Dehydrogenase (NADP(+)) 2) • CASP3 (Caspase 3) • CASP7 (Caspase 7)
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KRAS mutation • NRAS mutation • FLT3-ITD mutation • FLT3 mutation • KIT mutation • KRAS G13D • RAS mutation • NRAS Q61K • NRAS Q61 • KIT N822K • NRAS G12 • NRAS G13 • NRAS Q61L • NRAS G13D • NRAS G12C
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Venclexta (venetoclax) • Xospata (gilteritinib) • RMC-6236 • RMC-7977
1year
Farnesyltransferase (FTase) Inhibitors Increase Inhibition of KIT Mutants by Imatinib. (PubMed, Rep Biochem Mol Biol)
We found that farnesyltransferase inhibitors tipifarnib and lonafarnib, which inhibit RAS activity, inhibited ERK activation mediated by both wild-type and KIT mutants, which often occur in gastrointestinal stromal tumors. Similar to the primary KIT mutations, secondary mutations of KIT-induced ERK activation and cell response were inhibited by both inhibitors. Our results suggested the potential benefit of farnesyltransferase inhibitors either alone or combined with imatinib in the treatment of gastrointestinal stromal tumors carrying KIT mutations.
Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase)
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KIT mutation • KIT N822K • KIT V654A • KIT V560D • KIT W557
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imatinib • Zarnestra (tipifarnib)
over1year
Activity of Anlotinib in the Second-Line Therapy of Metastatic Gastrointestinal Stromal Tumors: A Prospective, Multicenter, In Vitro Study. (PubMed, Oncologist)
Anlotinib showed moderate antitumor activity in drug-resistant GIST cell lines in vitro, and good PFS and better tolerance in second-line therapy study.
Preclinical • Clinical Trial,Phase II • Journal • Stroma • Metastases
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KIT (KIT proto-oncogene, receptor tyrosine kinase)
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KIT mutation • KIT N822K • KIT exon 13 mutation • KIT V654A • KIT D820A
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imatinib • Focus V (anlotinib) • sunitinib
2years
New C3H Kit cancer mouse model develops late-onset malignant mammary tumors with high penetrance. (PubMed, Sci Rep)
This KIT variant corresponds to the N822K mutation found in human cancers, which is associated with imatinib-resistance...The disease model complements existing oncology research platforms. It allows for addressing the role of KIT mutations in breast cancer and identifying genetic and environmental modifiers of disease progression.
Preclinical • Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase)
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KIT mutation • KIT N822K
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imatinib
2years
Reinforced erythroid differentiation inhibits leukemogenic potential of t(8;21) leukemia. (PubMed, FASEB J)
Interestingly, in the AE9a murine model, a spontaneous step-wise erythroid differentiation path, as characterized by the differential expression of CD43/c-Kit and the upregulation of several key erythroid transcription factors (TFs), accompanied the decline or loss of leukemia-initiating potential. Notably, overexpression of one of the key erythroid TFs, Ldb1, potently disrupted the repopulation of AE9a leukemic cells in vivo, suggesting a new promising intervention strategy of t(8;21) AML through enforcing their erythroid differentiation.
Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase) • GATA1 (GATA Binding Protein 1) • SPN (Sialophorin)
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KIT N822K • KIT expression
over2years
Intratumoural heterogeneity with different resistant subclones in a treatment resistant gastrointestinal stromal tumour revealed through a novel tissue masking technology (ECP 2022)
Background & objectives: A 73-year-old man with a history of metastatic small bowel gastrointestinal stromal tumour (GIST) who have undergone liver and small bowel resections was found to have recurrent peritoneal nodules on follow-up despite being on Imatinib... This case demonstrated the utilization of Quantumcyte Oncomask, a novel tissue masking technology in detection of heterogeneous resistant subclones in a treatment resistant GIST. It enables the sampling of targeted areas in a tumour section to increase the cellular purity for molecular sequencing especially for the analysis of tumour heterogeneity which is known to be associated with therapeutic resistance. The presence of different mutation subclones in GIST is also important in guiding oncologists on the treatment choices.
ANO1 (Anoctamin 1)
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KIT mutation • KIT exon 11 mutation • KIT N822K • KIT exon 17 mutation • KIT N822Y
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imatinib
almost3years
Preclinical model-based evaluation of Imatinib resistance induced by KIT mutations and its overcoming strategies in gastrointestinal stromal tumor (GIST). (PubMed, Am J Transl Res)
We demonstrated the mechanism by which KIT secondary mutations on exon 13/17 cause Imatinib resistance to GIST, and validated that several novel TKIs were valuable therapeutic options against Imatinib-resistance for both secondary- and primary-KIT mutations.
Preclinical • Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase)
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KIT mutation • KIT exon 9 mutation • KIT N822K • KIT exon 13 mutation • KIT exon 17 mutation
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imatinib • sunitinib • Stivarga (regorafenib) • Ayvakit (avapritinib) • Qinlock (ripretinib)
3years
Genomic Analysis Focusing on RUNX1-RUNX1T1 in Japanese Patients with AML: HM-Screen-Japan 01 (ASH 2021)
AML with RUNX1-RUNX1T1 fusion gene is currently not indicated for transplantation in the first remission. Previous studies have demonstrated that approximately 30% of patients with CBF-AML harbored the KIT mutations at diagnosis, which might be an indicator of poor prognosis. In our study, the KIT mutations were detected much more frequently than in previously studies of newly-diagnosed CBF-AML.
Clinical
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FLT3 (Fms-related tyrosine kinase 3) • JAK2 (Janus kinase 2) • RUNX1 (RUNX Family Transcription Factor 1) • RUNX1T1 (RUNX1 Partner Transcriptional Co-Repressor 1)
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FLT3 mutation • FLT3 D835Y • FLT3 D835 • KIT N822K • KIT D816V • RUNX1-RUNX1T1 fusion • JAK2 V617F • JAK2 mutation
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FoundationOne® Heme CDx
almost4years
RUNX1/ETO and mutant KIT both contribute to programming the transcriptional and chromatin landscape in t(8;21) AML. (PubMed, Exp Hematol)
Global analysis of gene expression changes and alterations in the epigenome show that N822K-c-KIT expression profoundly influences the open chromatin landscape and transcription factor binding. However, our experiments also show that double mutant cells still differ from their patient derived counterparts, highlighting the importance of studying patient cells to obtain a true picture of how gene regulatory networks have been reprogrammed during tumourigenesis.
Journal
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FLT3 (Fms-related tyrosine kinase 3) • KIT (KIT proto-oncogene, receptor tyrosine kinase) • DNMT3A (DNA methyltransferase 1) • RUNX1 (RUNX Family Transcription Factor 1) • TET2 (Tet Methylcytosine Dioxygenase 2)
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TET2 mutation • KIT N822K • KIT expression
over4years
N822K- or V560G-mutated KIT activation preferentially occurs in lipid rafts of the Golgi apparatus in leukemia cells. (PubMed, Cell Commun Signal)
In AML, KIT mislocalizes to EL. Our findings, however, suggest that the mutant transduces phosphorylation signals on lipid rafts of the Golgi in leukemia cells. Unexpectedly, the KIT signal platform in MCL is similar to that of KIT in AML. These observations provide new insights into the pathogenic role of KIT mutants as well as that of other mutant molecules.
Journal
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KIT (KIT proto-oncogene, receptor tyrosine kinase)
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KIT mutation • KIT N822K • KIT D816V • KIT V560G