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Query: UMLS:C0029463 (
osteosarcoma
)
16,637
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A single, nonlethal dose of actinomycin D will cause total regression and cure of Ridgway
osteogenic sarcoma
in mice. A cure is not obtained with a single dose daily for 7 days, a dose regimen which kills 10% of normal C57BL/6 X
DBA
/2 mice. This suggests that actinomycin D is more effective on a single high-dose schedule than on chronic daily therapy. Analysis of drug exposure in Ridgway
osteogenic sarcoma
and normal mouse tissues following the single and multiple-dose regimens suggests the difference in therapeutic response is due to drug exposure at a higher concentration in Ridgway
osteogenic sarcoma
after the single high dose than after the multiple-dose regimen. This may be related to the higher drug concentration attained in blood following the single-dose regimen than is attained with the multidose regimen.
...
PMID:Disposition of [3H]actinomycin D in tumor-bearing mice. 106 63
Flavone acetic acid (FAA) is a new antitumor agent with broad activity against transplantable solid tumors of mice but with only scant or no activity against leukemias and lymphomas. The technique of alkaline elution was used to study DNA lesions in s.c. implanted Glasgow
osteogenic sarcoma
in C57BL/6 x
DBA
/2 F1 mice treated i.v. with FAA. At efficacious dosages (235 and 200 mg/kg), FAA produced extensive single strand breakage. Formation of single strand breaks was dependent on time of assay after exposure to FAA with only minimal damage occurring prior to 5 h posttreatment. Apparently Glasgow
osteogenic sarcoma
had no capacity to repair single strand breaks for at least 45 h after drug administration. Thus, FAA differs in its mechanism from other scission agents (e.g., VP-16). Neither interstrand cross-links nor DNA-protein cross-links were detected. DNA single strand breaks did not occur in the bone marrow cells or in the unresponsive P388 leukemia cells at dosages causing extensive DNA damage in solid tumor cells.
...
PMID:Flavone acetic acid (NSC 347512)-induced DNA damage in Glasgow osteogenic sarcoma in vivo. 342 92
Diamond Blackfan anemia
(
DBA
) is a rare disease characterized by aplasia or hypoplasia of erythroid lineage. Normochromic, usually macrocytic, but occasionally normocytic anemia and reticulocytopenia are characteristic findings of
DBA
.
DBA
is associated with an increased risk of malignancy. Most of the reported malignancies are acute myeloid leukemia. Solid tumors including hepatocellular carcinoma and
osteosarcoma
have also been identified. We could find 29 reported cases with
DBA
and malignancy. Two of them were diagnosed as Hodgkin lymphoma at 15 and 23 years, respectively. Here we report a 7-year-old boy with
DBA
who developed Hodgkin disease.
...
PMID:Hodgkin lymphoma in a child with Diamond Blackfan anemia. 1667 21
The gene encoding the small subunit ribosomal protein 19 (RPS19) is mutated in about 25% of cases of the bone marrow failure syndrome
Diamond Blackfan Anemia
(
DBA
), a childhood disease characterized by failure of red cell production. In these cases
DBA
is inherited as an autosomal dominant trait and RPS19 haploinsufficiency is thought to cause the disease. To study the molecular pathogenesis of
DBA
we used siRNA to decrease the level of RPS19 in two human cell lines, HeLa cells and U-2 OS
osteosarcoma
cells. Cells with reduced RPS19 levels showed a dramatic reduction in the amounts of small 40S ribosome subunits and mature 80S ribosomes and an excess of large 60S subunits. These cells were defective in 18S rRNA production and accumulated 21S and 20S nuclear pre-rRNA molecules, suggesting that RPS19 is required for specific steps in rRNA processing. RPS19 depletion produced a reduction in steady-state levels of RPS6 and RPS16 via a post-transcriptional mechanism while the levels of RPL7 and RPL26 were unaltered, indicating that levels of ribosomal proteins are determined by subunit assembly. This has interesting implications for the pathogenesis of
DBA
suggesting that deficiency of any of the RPS proteins might have a similar effect and thus may be responsible for causing
DBA
. Finally in cell lines from
DBA
patients with mutations we find increased levels of 21S rRNA precursors but no abnormality in the ribosome profile on sucrose gradients or in the steady-state levels of RPS19 suggesting that some cells can partially compensate for the loss of one allele of RPS19. We conclude that defects in ribosome biogenesis may underlie the pathology of
Diamond Blackfan Anemia
.
...
PMID:Cells depleted for RPS19, a protein associated with Diamond Blackfan Anemia, show defects in 18S ribosomal RNA synthesis and small ribosomal subunit production. 1737 18
The inherited bone marrow failure syndromes are traditionally considered to be pediatric disorders, but in fact, many of the patients now are diagnosed as adults, and many diagnosed as children now live to reach adulthood. The most common of these rare disorders include Fanconi anemia, dyskeratosis congenita, Shwachman-Diamond syndrome and amegakaryocytic thrombocytopenia, which often develop aplastic anemia and may evolve into myelodysplastic syndrome and acute myeloid leukemia; and
Diamond-Blackfan anemia
, severe congenital neutropenia, and thrombocytopenia absent radii, single cytopenias that rarely if ever become aplastic but have increased risks of leukemia. In addition, the first three syndromes have high risks of solid tumors: head and neck and anogenital squamous cell carcinoma in Fanconi anemia and dyskeratosis congenita, and
osteogenic sarcoma
in
Diamond-Blackfan anemia
. Diagnosis of a marrow failure syndrome requires recognition of characteristic physical abnormalities when present, and consideration of these disorders in the differential diagnosis of patients who present with "acquired" aplastic anemia, myelodysplastic syndrome, acute myeloid leukemia, or atypically early cancers of the types seen in the syndromes. Ultimate proof will come from identification of pathogenic mutations in genes associated with each syndrome.
...
PMID:Diagnosis, genetics, and management of inherited bone marrow failure syndromes. 1802 6
Diamond Blackfan anemia
(
DBA
) is an inherited bone marrow failure syndrome characterized by red cell aplasia and congenital anomalies. A predisposition to cancer has been suggested but not quantified by case reports. The
DBA
Registry of North America (DBAR) is the largest established
DBA
patient cohort, with prospective follow-up since 1991. This report presents the first quantitative assessment of cancer incidence in
DBA
. Among 608 patients with 9458 person-years of follow-up, 15 solid tumors, 2 acute myeloid leukemias, and 2 cases of myelodysplastic syndrome were diagnosed at a median age of 41 years in patients who had not received a bone marrow transplant. Cancer incidence in
DBA
was significantly elevated. The observed-to- expected ratio for all cancers combined was 5.4 (P < .05); significant observed-to-expected ratios were 287 for myelodysplastic syndrome, 28 for acute myeloid leukemia, 36 for colon carcinoma, 33 for
osteogenic sarcoma
, and 12 for female genital cancers. The median survival was 56 years, and the cumulative incidence of solid tumor/leukemia was approximately 20% by age 46 years. As in Fanconi anemia and dyskeratosis congenita,
DBA
is both an inherited bone marrow failure syndrome and a cancer predisposition syndrome; cancer risks appear lower in
DBA
than in Fanconi anemia or dyskeratosis congenita. This trial was registered at www.clinicaltrials.gov as #NCT00106015.
...
PMID:Incidence of neoplasia in Diamond Blackfan anemia: a report from the Diamond Blackfan Anemia Registry. 2236 38
Three children treated with bone marrow transplantation for acute lymphoblastic leukemia,
Diamond-Blackfan anemia
, and congenital amegakaryocytic thrombocytopenia developed secondary
osteosarcoma
in the left tibia at the age of 13, 13, and 9 years, respectively, at 51, 117, and 106 months after transplantation, respectively. Through treatment with chemotherapy and surgery, all 3 patients are alive without disease. We surveyed the literature and reviewed 10 cases of
osteosarcoma
after hematopoietic stem cell transplantation (SCT), including our 3 cases. Eight of the patients had received myeloablative total body irradiation before SCT. The mean interval from SCT to the onset of
osteosarcoma
was 6 years and 4 months, and the mean age at the onset of
osteosarcoma
was 14 years and 5 months. The primary site of the post-SCT
osteosarcoma
was the tibia in 6 of 10 cases, in contrast to de novo
osteosarcoma
, in which the most common site is the femur. At least 7 of the 10 patients are alive without disease.
Osteosarcoma
should be one of the items for surveillance in the follow-up of patients who undergo SCT.
...
PMID:Osteosarcoma after bone marrow transplantation. 2392 19
Mouse double minute 2 (Mdm2) is a multifaceted oncoprotein that is highly regulated with distinct domains capable of cellular transformation. Loss of Mdm2 is embryonically lethal, making it difficult to study in a mouse model without additional genetic alterations. Global overexpression through increased Mdm2 gene copy number (Mdm2
Tg
) results in the development of hematopoietic neoplasms and sarcomas in adult animals. In these mice, we found an increase in osteoblastogenesis, differentiation, and a high bone mass phenotype. Since it was difficult to discern the cell lineage that generated this phenotype, we generated osteoblast-specific Mdm2 overexpressing (Mdm2
TgOb
) mice in 2 different strains, C57BL/6 and
DBA
. These mice did not develop malignancies; however, these animals and the MG63 human
osteosarcoma
cell line with high levels of Mdm2 showed an increase in bone mineralization. Importantly, overexpression of Mdm2 corrected age-related bone loss in mice, providing a role for the proto-oncogenic activity of Mdm2 in bone health of adult animals.
...
PMID:The proto-oncogene function of Mdm2 in bone. 3001 Oct 84
Osteosarcoma
(OS) is the most frequent primary bone cancer in children and adolescents and the third most frequent in adults. Many inherited germline mutations are responsible for syndromes that predispose to osteosarcomas including Li Fraumeni syndrome, retinoblastoma syndrome, Werner syndrome, Bloom syndrome or
Diamond-Blackfan anemia
.
TP53
is the most frequently altered gene in
osteosarcoma
. Among other genes mutated in more than 10% of OS cases, c-Myc plays a role in OS development and promotes cell invasion by activating MEK-ERK pathways. Several genomic studies showed frequent alterations in the
RB
gene in pediatric OS patients.
Osteosarcoma
driver mutations have been reported in
NOTCH1
,
FOS
,
NF2
,
WIF1
,
BRCA2
,
APC
,
PTCH1
and
PRKAR1A
genes. Some miRNAs such as miR-21, -34a, -143, -148a, -195a, -199a-3p and -382 regulate the pathogenic activity of MAPK and PI3K/Akt-signaling pathways in
osteosarcoma
. CD133+
osteosarcoma
cells have been shown to exhibit stem-like gene expression and can be tumor-initiating cells and play a role in metastasis and development of drug resistance. Although currently
osteosarcoma
treatment is based on adriamycin chemoregimens and surgery, there are several potential targeted therapies in development. First of all, activity and safety of cabozantinib in
osteosarcoma
were studied, as well as sorafenib and pazopanib. Finally, novel bifunctional molecules, of potential imaging and
osteosarcoma
targeting applications may be used in the future.
...
PMID:Molecular Biology of Osteosarcoma. 3275 22
