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Target Concepts:
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Query: UMLS:C0026986 (
myelodysplastic syndrome
)
14,926
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Myelodysplastic syndromes
and acute myeloid leukemia with
TP53
mutations are characterized by frequent relapses, poor or short responses, and poor survival with the currently available therapies including chemotherapy and 5-azacitidine (AZA). PRIMA-1
Met
(
APR
-246,
APR
) is a methylated derivative of PRIMA-1, which induces apoptosis in human tumor cells through restoration of the transcriptional transactivation function of mutant p53. Here we show that low doses of
APR
on its own or in combination with AZA reactivate the p53 pathway and induce an apoptosis program. Functionally, we demonstrate that
APR
exerts these activities on its own and that it synergizes with AZA in
TP53
-mutated
myelodysplastic syndromes
(
MDS
)/acute myeloid leukemia (AML) cell lines and in
TP53
-mutated primary cells from
MDS
/AML patients. Low doses of
APR
on its own or in combination with AZA also show significant efficacy
in vivo
Lastly, using transcriptomic analysis, we found that the
APR
+ AZA synergy was mediated by downregulation of the FLT3 pathway in drug-treated cells. Activation of the FLT3 pathway by FLT3 ligand reversed the inhibition of cell proliferation by
APR
+ AZA. These data suggest that
TP53
-mutated
MDS
/AML may be better targeted by the addition of
APR
-246 to conventional treatments.
...
PMID:Synergistic effects of PRIMA-1
Met
(APR-246) and 5-azacitidine in
TP53
-mutated myelodysplastic syndromes and acute myeloid leukemia. 3148 57
For most patients with higher-risk
myelodysplastic syndromes
(HR-MDS) the hypomethylating agents (HMA) azacitidine and decitabine remain the mainstay of therapy. However, the prognosis mostly remains poor and aside from allogeneic hematopoietic stem cell transplantation no curative treatment options exist. Unlike acute myeloid leukemia, which has seen a dramatic expansion of available therapies recently, no new agents have been approved for
MDS
in the United States since 2006. However, various novel HMAs, HMA in combination with venetoclax, immune checkpoint inhibitors, and targeted therapies for genetically defined patient subgroups such as
APR
-246 or IDH inhibitors, have shown promising results in early stages of clinical testing. Furthermore, the wider availability of genetic testing is going to allow for a more individualized treatment of
MDS
patients. Herein, we review the current treatment approach for HR-
MDS
and discuss recent therapeutic advances and the implications of genetic testing on management of HR-
MDS
.
...
PMID:Following in the footsteps of acute myeloid leukemia: are we witnessing the start of a therapeutic revolution for higher-risk myelodysplastic syndromes? 3242 3
RAS, TP53 (p53) and MYC are among the most frequently altered driver genes in cancer. Thus, RAS is the most frequently mutated oncogene, MYC the most frequently amplified gene and TP53 the most frequently mutated tumor suppressor gene and overall the most frequently mutated gene in cancer. Theoretically, therefore, these genes are highly attractive targets for cancer treatment. However, as the protein products of each of these genes lack an accessible hydrophobic pocket into which low molecular weight compounds might bind with high affinity, they have proved difficult to target and have traditionally been referred to as "undruggable." Despite this branding, several low molecular weight compounds targeting each of these proteins have recently been reported to have anticancer activity in preclinical models. Indeed, several drugs inhibiting mutant KRAS, MYC overexpression or reactivating mutant p53 have undergone or are currently undergoing clinical trials. For targeting mutant KRAS and reactivating mutant p53, trials have progressed to a Phase III stage, that is, the mutant-p53 reactivating drug,
APR
-246 is currently being investigated in patients with
myelodysplastic syndrome
(
MDS
) and the RAS inhibitor, rigosertib is also undergoing evaluation in patients with
MDS
. Although there appears to be no directly acting MYC inhibitor currently being tested in a clinical trial, an anti-MYC compound, known as OmoMYC has been extensively validated in multiple preclinical models and is being developed for clinical evaluation. Based on current evidence, the traditional perception of RAS, p53 and MYC as being "undruggable" would appear to be coming to an end.
...
PMID:Drugging "undruggable" genes for cancer treatment: Are we making progress? 3263 80
