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Query: KEGG:D03229 (
BLM
)
1,348
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Bloom syndrome (BS) is a rare autosomal recessive genetic disorder characterized by growth deficiency, unusual facies, sun-sensitive telangiectatic erythema,
immunodeficiency
and predisposition to cancer. The causative gene for BS is the
BLM
gene which encodes the
BLM
RecQ helicase protein. The
BLM
gene has 4437 bp and encodes 1417 amino acids. The detection of
BLM
gene mutations for laboratory diagnosis of BS is laborious and impractical, unless there are common mutations in a population. Here we describe the immunoblot and immunohistochemical analyses for the detection of the BLM protein using a polyclonal
BLM
antibody. The
BLM
gene and protein were consistently and clearly detected in Epstein-Barr virus (EBV)-transformed or phytohemagglutinin (PHA)-stimulated lymphoblasts from control and various human hematopoietic cell lines. In a 7-week old human fetal brain, the
BLM
gene expression was strongly detected in contrast to an adult human brain. The BLM protein was not detected in EBV-transformed lymphoblasts from three BS patients. By immunohistochemistry, nuclear dots of the BLM protein were detected in both EBV-transformed lymphoblasts and PHA-stimulated lymphoblasts from the control. However, in lymphoblasts from BS patients no nuclear dots of the BLM protein were detected. These results indicate that the combinational analysis of immunoblotting and immunohistochemistry is a useful approach to screening of BS, although a mutation analysis is necessary for a definitive diagnosis of BS.
...
PMID:Expression of BLM (the causative gene for Bloom syndrome) and screening of Bloom syndrome. 1206 Aug 58
Treatment of patients with primary mediastinal B-cell lymphoma (PMBCL) remains controversial. We started a controlled clinical trial to evaluate the efficacy and toxicity of a conventional versus more intensive regimen of combined chemotherapy followed by radiotherapy to the mediastinum with the mantle technique. From 1989 to 1997, 68 patients diagnosed with previously untreated PMBCL, aged 18-65 years and negative for
immunodeficiency
virus test, were considered candidates to receive either conventional chemotherapy with CEOP-
Bleo
(cyclophosphamide 750 mg/m(2), vincristine 1.4 mg/m(2), prednisone 40 mg/m(2), epirubicin 70 mg/m(2), and bleomycin 10 mg/m(2)) or mega CEOP-
Bleo
(cyclophosphamide 1000 mg/m(2), epirubicin 120 mg/m(2), vincristine, prednisone, and bleomycin at the same doses) every 21 days for six cycles, followed by radiotherapy to the mediastinum with the mantle technique (35-45 Gy, mean 38 Gy). Complete response (CR) rates were not statistically different: 64% [95 percent confidence interval (CI): 58 percent to 70 percent] for conventional arm vs 81 percent (95 CI: 77-86 percent) in the intensive group (p=0.2). However, failure-free survival (FFS) and overall survival (OS) had statistical differences. At 5 years, actuarial FFS for patients treated with conventional chemotherapy was 51 percent (95 percent CI: 44-59 percent) compared to 70 percent (95 percent CI: 65-76 percent) in the intensive arm (p>0.01). OS rates were also different: 54 percent (95 percent CI: 48-57 percent) vs 70 percent (95 percent CI: 65-76 percent), respectively (p<0.01). Toxicity was mild and no therapy-related deaths were observed. At a median follow-up of 7.3 years, no second neoplasia or acute leukemia has been observed. The international prognostic index was not useful to define clinical risk in this selected group of patients. Multivariate analysis identified pleural and pericardial effusion and chemotherapy regimen as prognostic factors influencing FFS and OS. We feel that patients with PMBCL should be treated with more intensive, but not myeloablative chemotherapy, followed by adjuvant radiotherapy to achieve an improvement in outcome in this setting of patients. Patients with pleural or pericardial effusion are considered at high risk for failure with the actual programs of treatment and probably will be considered for experimental therapeutic approaches.
...
PMID:Combined therapy in the treatment of primary mediastinal B-cell lymphoma: conventional versus escalated chemotherapy. 1218 5
Bloom syndrome (BS) is a genetic disorder associated with dwarfism,
immunodeficiency
, reduced fertility, and an elevated risk of cancer. To investigate the mechanism of this disease, we isolated from human HeLa extracts three complexes containing the helicase defective in BS,
BLM
. Interestingly, one of the complexes, termed BRAFT, also contains five of the Fanconi anemia (FA) complementation group proteins (FA proteins). FA resembles BS in genomic instability and cancer predisposition, but most of its gene products have no known biochemical activity, and the molecular pathogenesis of the disease is poorly understood. BRAFT displays a DNA-unwinding activity, which requires the presence of
BLM
because complexes isolated from
BLM
-deficient cells lack such an activity. The complex also contains topoisomerase IIIalpha and replication protein A, proteins that are known to interact with
BLM
and could facilitate unwinding of DNA. We show that
BLM
complexes isolated from an FA cell line have a lower molecular mass. Our study provides the first biochemical characterization of a multiprotein FA complex and suggests a connection between the
BLM
and FA pathways of genomic maintenance. The findings that FA proteins are part of a DNA-unwinding complex imply that FA proteins may participate in DNA repair.
...
PMID:A multiprotein nuclear complex connects Fanconi anemia and Bloom syndrome. 1272 1
Bloom syndrome and ataxia-telangiectasia are autosomal recessive human disorders characterized by
immunodeficiency
, genome instability and predisposition to develop cancer. Recent data reveal that the products of these two genes,
BLM
and ATM, interact and function together in recognizing abnormal DNA structures. To investigate the function of these two molecules in DNA damage recognition, we generated double knockouts of ATM(-/-)
BLM
(-/-) in the DT40 chicken B-lymphocyte cell line. The double mutant cells were viable and exhibited a variety of characteristics of both ATM(-/-) and
BLM
(-/-) cells. There was no evidence for exacerbation of either phenotype; however, the more extreme radiosensitivity seen in ATM(-/-) and the elevated sister chromatid exchange seen in
BLM
(-/-) cells were retained in the double mutants. These results suggest that ATM and
BLM
have largely distinct roles in recognizing different forms of damage in DNA, but are also compatible with partially overlapping functions in recognizing breaks in radiation-damaged DNA.
...
PMID:Disruption of the BLM gene in ATM-null DT40 cells does not exacerbate either phenotype. 1498
Bloom syndrome is a rare autosomal recessive genetic disorder characterized by growth deficiency, unusual facies, sun-sensitive telangiectatic erythema,
immunodeficiency
and predisposition to cancer. The causative gene for Bloom syndrome is
BLM
, which encodes the
BLM
RecQ helicase homolog protein. The first part of this review describes a long-term follow-up study of two Bloom syndrome siblings. Subsequently, the focus is placed on the functional domains of
BLM
. Laboratory diagnosis of Bloom syndrome by detecting mutations in
BLM
is laborious and impractical, unless there are common mutations in a population. Immunoblot and immunohistochemical analyses for the detection of the BLM protein using a polyclonal
BLM
antibody, which are useful approaches for clinical diagnosis of Bloom syndrome, are also described. In addition, a useful adjunct for the diagnosis of Bloom syndrome in terms of the
BLM
function is investigated, since disease cells must have the defective
BLM
helicase function. This review also discusses the nuclear localization signal of
BLM
, the proteins that interact with
BLM
and tumors originating from Bloom syndrome.
...
PMID:Clinical features of Bloom syndrome and function of the causative gene, BLM helicase. 1513 5
Bloom syndrome is a rare autosomal recessive genetic disorder characterized by lupus-like erythematous telangiectasias of the face, sun sensitivity, stunted growth, and
immunodeficiency
. Chromosome instability syndromes have a common feature, being associated at high frequency with neoplasia. BS is considered as one of the chromosome instability syndromes since the fibroblasts or lymphocytes of BS patients show excessive spontaneous chromosome instability. The causative gene of BS (
BLM
) was identified as a RecQ helicase homologue. In this review, we showed the characteristic phenotypes of BS, especially two Japanese siblings. In the latter of the review, the functional domains of
BLM
, those are nuclear localization signal and the interacting proteins such as ATM, are shown. Several lines of reports indicates that
BLM
helicase is involved in the re-initiation of DNA replication at sites where replication forks have arrested or collapsed. To elucidate the precise function of RecQ helicase in DNA repair and replication aims not only to improve our understanding of the molecular basis for tumorigenesis, but also to extend the range of potential therapeutic targets.
...
PMID:The function of RecQ helicase gene family (especially BLM) in DNA recombination and joining. 1547 92
Bloom syndrome is a rare autosomal recessive genetic disorder characterized by lupus-like erythematous telangiectasias of the face, sun sensitivity, stunted growth, and
immunodeficiency
. Chromosome instability syndromes have a common feature, being associated at high frequency with neoplasia. BS is considered as one of the chromosome instability syndromes since the fibroblasts or lymphocytes of BS patients show excessive spontaneous chromosome instability. The causative gene of BS (
BLM
) was identified as a RecQ helicase homologue. In this review, we showed the characteristic phenotypes of BS, especially two Japanese siblings. In the latter of the review, the functional domains of
BLM
, those are nuclear localization signal and the interacting proteins such as ATM, are shown. Several lines of reports indicates that
BLM
helicase is involved in the re-initiation of DNA replication at sites where replication forks have arrested or collapsed. To elucidate the precise function of RecQ helicase in DNA repair and replication aims not only to improve our understanding of the molecular basis for tumorigenesis, but also to extend the range of potential therapeutic targets.
...
PMID:The function of RecQ helicase gene family (especially BLM) in DNA recombination and joining. 1549 27
In HIV infection, continuous immune activation leads to accelerated ageing of the adaptive immune system, similar to that observed in elderly people. We investigated the expression of WRN and
BLM
(genes involved in disorders characterized by premature ageing, genomic instability and cancer predisposition) in peripheral blood mononuclear cells (PBMC) activated in vitro with phytohaemagglutinin (PHA) and infected with different HIV-1 strains. The steady state levels of mRNA were analysed by reverse transcription-polymerase chain reaction (RT-PCR), and protein expression was assayed using immunocytochemistry and Western blot techniques. In uninfected PBMC, PHA stimulation induced an increase in
BLM
mRNA and protein expression, while WRN expression remained virtually unchanged. When PBMC were infected in vitro with a lymphotropic HIV-1 strain, the level of
BLM
mRNA showed a peak at 24 h of infection, followed by a decline to uninfected culture levels. A similar result failed to be seen using an R5-tropic HIV-1 strain. In accordance with mRNA expression, in HIV-infected cultures PBMC were stained more frequently and more intensely by a
BLM
-specific antibody as compared to uninfected cultures, staining peaking at 24. Conversely, WRN expression was not modulated by HIV-1. The proportion of cells showing
BLM
up-regulation, established by immunocytochemical staining, was much greater than the proportion of productively infected PBMC, as established by proviral DNA measurement. This result indicates that
BLM
up-regulation is probably a result of an indirect bystander cell effect. Activation of the
BLM
gene in infected PBMC suggests that premature ageing could be a further immunopathogenetic mechanism involved in HIV-induced
immunodeficiency
, and points to a possible new candidate target for innovative therapeutic intervention.
...
PMID:Expression of Werner and Bloom syndrome genes is differentially regulated by in vitro HIV-1 infection of peripheral blood mononuclear cells. 1549 34
Bloom's syndrome (BS) is a rare human genetic disorder characterized by dwarfism,
immunodeficiency
, genomic instability and cancer predisposition. We have previously purified three complexes containing
BLM
, the helicase mutated in this disease. Here we demonstrate that BLAP75, a novel protein containing a putative OB-fold nucleic acid binding domain, is an integral component of
BLM
complexes, and is essential for their stability in vivo. Consistent with a role in
BLM
-mediated processes, BLAP75 colocalizes with
BLM
in subnuclear foci in response to DNA damage, and its depletion impairs the recruitment of
BLM
to these foci. Depletion of BLAP75 by siRNA also results in deficient phosphorylation of
BLM
during mitosis, as well as defective cell proliferation. Moreover, cells depleted of BLAP75 display an increased level of sister-chromatid exchange, similar to cells depleted of
BLM
by siRNA. Thus, BLAP75 is an essential component of the
BLM
-associated cellular machinery that maintains genome integrity.
...
PMID:BLAP75, an essential component of Bloom's syndrome protein complexes that maintain genome integrity. 1577 63
The mutations of
BLM
gene may result in Bloom's syndrome which includes
immunodeficiency
, predisposition to malignant tumors and so on, and enhances sister chromati exchange (SCE), DNA replication failure, genome instability, and increases cancer susceptibility. This study was aimed to investigate the variability of mRNA expression level and cDNA structure of
BLM
gene in tumor cell strains so as to look for a new cancerogenic mechanism and to find a new therapeutic target. The expression level of mRNA and the structure of cDNA of
BLM
gene in six tumor cell strains and the normal human bone marrow mononuclear cells were detected with RT-PCR and DNA sequencing was performed. The results indicated that these tumors cells expressed
BLM
mRNA higher than the normal human bone marrow mononuclear cells (P < 0.01), but no cDNA sequence abnormality of
BLM
gene in these tumors cells was observed. It is concluded that the increase of expressing level of
BLM
mRNA may play an important role in the development of these tumors.
...
PMID:[Expression of BLM mRNA in six tumor cell strains]. 1627 51
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