Evidence against a direct cytotoxic effect of alpha interferon and zidovudine in HTLV-I associated adult T cell leukemia/lymphoma

Bazarbachi, Ali; Nasr, Rihab; El-Sabban, ME; Mahé, A.; Mahieux, Renaud; Gessain, Antoine; Darwiche, Nadine; Dbaibo, Ghassan; Kersual, Joëlle; Zermati, Yaël; Dianoux, Laurent; Mk, Chelbi-Alix; Hermine, Olivier

doi:10.1038/sj.leu.2401742

Cited by 66 publications

(59 citation statements)

References 12 publications

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“…70 For example, in patients with HTLV-1-associated myelopathy (HAM), reduction of HTLV-1 viral DNA load was reported during treatment with the reverse transcriptase inhibitor lamivudine, 71 and HTLV-1 replication was inhibited by the nucleoside reverse-transcriptase inhibitors tenofovir, abacavir, lamivudine, zalcitabine, stavudine, zidovudine and didanosine. 72,73 Another report described the successful treatment of a patient with ATL using zidovudine, lamivudine and IFN-a.…”

Section: New Chemical Anti-tumor Agents 1) Antiretroviral Therapymentioning

confidence: 99%

Treatment of Adult T-cell Leukemia

Uozumi

2010

J Clin Exp Hematopathol

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Adult T-cell Leukemia (ATL) is an aggressive malignant disease of CD4 + T-cells associated with human T-cell leukemia virus type I (HTLV-I). Prognosis of ATL patients is directly correlated to the subtype of ATL. Treatment of the aggressive forms (acute and lymphoma types) of ATL remains inadequate, as most ATL patients receive conventional chemotherapy without stem cell rescue. At present, LSG15 is the standard chemotherapy for the treatment of aggressive ATL, but the efficacy of LSG15 in most patients is transient. To prolong median survival time, additional therapies for maintenance of complete response (CR) are needed after achieving CR by induction chemotherapy. Improved outcome after allogeneic stem cell transplantation (allo-SCT), despite a high incidence of graft-versus-host disease, has been reported. Thus, allogeneic bone marrow transplantation and allogeneic peripheral blood SCT may have great potential for eradication of HTLV-1 and cure of ATL. Recently, reduced-intensity conditioning stem cell transplantation was also reported to be effective for ATL. Although several issues, including selection criteria for patients and sources of stem cells remain to be resolved, allo-SCT may be considered as a treatment option for patients with aggressive ATL. To evaluate whether allo-SCT is more effective than the standard chemotherapy (LSG15) for aggressive ATL, an upfront phase II clinical trial of JCOG-LSG is now being planned. Novel innovative targeted strategies, such as antiretroviral therapy, arsenic trioxide, nuclear factor-kB inhibitors, proteasome inhibitors, histone deacetylase inhibitors, several monoclonal antibodies including anti-CC chemokine receptor 4, anti-folate, purine nucleotide phosphorylase inhibitor, mTOR (mammalian target of rapamycin) inhibitor, bendamustine, small molecule Bcl-2 inhibitors and Tax-targeted immunotherapy, should be promptly studied in order to develop curative treatments for ATL in the near future. 〔J Clin Exp Hematopathol 50(1) : 9-25, 2010〕

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Section: New Chemical Anti-tumor Agents 1) Antiretroviral Therapymentioning

confidence: 99%

Treatment of Adult T-cell Leukemia

Uozumi

2010

J Clin Exp Hematopathol

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“…The best studied exemple is another leukemia, acute T cell leukemia (ATL), where infection by a virus, HTLV-I leads to the expression of a virally encoded transactivator protein, Tax that activates a large number of cellular genes, including the NF-kB survival pathway and an IL2 autocrine loop. Arsenic will induce the death of these cells (Bazarbachi et al, 1999) and tax catabolism through the proteasome (ElSabban et al, 2000). Arrays analyses demonstrate that most of the genes rapidly down-regulated by arsenic are indeed NF-kB targets, implying that Tax degradation rapidly shuts o this network of anti-apoptotic genes and providing a plausible explanation for cell death induction (A Bazarbachi and H de TheÂ , manuscript in preparation).…”

Section: Synergy or Antagonism Or Ra/arsenic Associations?mentioning

confidence: 99%

Pathways of retinoic acid- or arsenic trioxide-induced PML/RARα catabolism, role of oncogene degradation in disease remission

Zhu

Lallemand-Breitenbach

2001

Oncogene

147

130

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Although there is evidence to suggest that PML/RARa expression is not the sole genetic event required for the development of acute promyelocytic leukemia (APL), there is little doubt that the fusion protein plays a central role in the initiation of leukemogenesis. The two therapeutic agents, retinoic acid and arsenic, that induce clinical remissions in APL, both target the oncogenic fusion protein, representing the ®rst example of oncogene-directed cancer therapy. This review focuses on the molecular mechanisms accounting for PML/RARa degradation. Each drug targets a speci®c moiety of the fusion protein (RARa for retinoic acid, PML for arsenic) to the proteasome. Moreover, both activate a common caspase-dependent cleavage in the PML part of the fusion protein. Speci®c molecular determinants (the AF2 transactivator domain of RARa for retinoic acid and the K160 SUMO-binding site in PML for arsenic) are respectively implicated in RA-or arsenic-triggered catabolism. The respective roles of PML/RARa activation versus its catabolism are discussed with respect to di erentiation or apoptosis induction in the context of single or dual therapies. Oncogene (2001) 20, 7257 ± 7265.

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“…As 2 O 3 show promising results in the treatment of patients with ATL in combination with interferon (IFN)-a. [3][4][5][6][7][8] Although As 2 O 3 -induced apoptosis is thought to play a major role in its observed therapeutic growth inhibitory effects in treating ATL 9,10) the effects of As 2 O 3 on HTLV-1 infection/transmission have not been reported.HTLV-1 can be distinguished from all other retroviruses on the basis of the infection process: it is transmitted almost exclusively via cell-to-cell contact and cell-to-cell fusion (also termed syncytium formation), and the free viral particle is very poorly infectious.11) The HTLV-1 envelope glycoprotein is synthesized as a 61-kDa precursor that is cleaved into cellsurface (gp46) and transmembrane (gp21) proteins 12,13) and the gp46 product is thought to play an important role as the virus attachment protein. HTLV-1 can induce syncytium formation between infected cells and certain uninfected cell types 14,15) but this process can be blocked by antibodies against the gp46 protein or against gp46-derived peptides.…”

mentioning

confidence: 99%

mentioning

confidence: 99%

Arsenic Trioxide Inhibits Human T Cell-Lymphotropic Virus-1-Induced Syncytiums by Down-Regulating gp46

Nabeshi

Yoshikawa

Kamada

et al. 2009

Biological & Pharmaceutical Bulletin

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Human T-cell leukemia virus type 1 (HTLV-1) is the etiologic agent of adult T-cell leukemia (ATL).1,2) ATL is characterized by malignant lympho-proliferation of mature activated T cells, predominantly CD4-positive T cells. This proliferation develops after a long period of latency following HTLV-1 infection. It is currently estimated that there are about twenty million HTLV-1 carriers worldwide. Of these, around 5% are at risk for ATL onset, and it has been reported that the incidence of ATL has been increasing. Epidemiological studies have indicated strongly that an increased HTLV-1 virus load is an important factor in ATL onset, although the detailed mechanisms of ATL onset are unknown. Therefore, an ideal anti-ATL agent would have both a growth inhibitory effect on ATL cells and an inhibitory effect on transmission of HTLV-1-infected cells. As 2 O 3 show promising results in the treatment of patients with ATL in combination with interferon (IFN)-a. [3][4][5][6][7][8] Although As 2 O 3 -induced apoptosis is thought to play a major role in its observed therapeutic growth inhibitory effects in treating ATL 9,10) the effects of As 2 O 3 on HTLV-1 infection/transmission have not been reported.HTLV-1 can be distinguished from all other retroviruses on the basis of the infection process: it is transmitted almost exclusively via cell-to-cell contact and cell-to-cell fusion (also termed syncytium formation), and the free viral particle is very poorly infectious.11) The HTLV-1 envelope glycoprotein is synthesized as a 61-kDa precursor that is cleaved into cellsurface (gp46) and transmembrane (gp21) proteins 12,13) and the gp46 product is thought to play an important role as the virus attachment protein. HTLV-1 can induce syncytium formation between infected cells and certain uninfected cell types 14,15) but this process can be blocked by antibodies against the gp46 protein or against gp46-derived peptides. 16,17) Thus, gp46 is a key protein for HTLV-1 transmission via syncytium formation, which is a critical process for HTLV-1 transmission via cell-to-cell contact.In the present study, we reveal that HTLV-1-induced syncytium formation can be blocked by As 2 O 3 treatment. Western blot analysis indicated that gp46 was down-regulated by As 2 O 3 treatment. Our results suggest that As 2 O 3 can prevent the HTLV-1 transmission by reducing levels of gp46, in addition to its therapeutic effect on ATL by promoting apoptosis. These results suggested that As 2 O 3 may open new avenues for treating HTLV-1-related diseases, including ATL. MATERIALS AND METHODS Cell CultureThe HTLV-1-infected cell line MT-2 (a kind gift from Hayashibara Biochemical Laboratories, Inc.) was grown in RPMI-1640 (Wako Pure Chemical Industries, Ltd., Osaka, Japan) supplemented with 10% heat-inactivated fetal calf serum and 1% Antibiotic-Antimycotic Mix stock solution (Nacalai Tesque, Osaka, Japan) in a humidified atmosphere of 95% air/5% CO 2 , at 37°C. A HeLa cell line was maintained in minimum essential medium (MEM-a; Wako) supplemented with 10% heat-...

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Evidence against a direct cytotoxic effect of alpha interferon and zidovudine in HTLV-I associated adult T cell leukemia/lymphoma

Cited by 66 publications

References 12 publications

Treatment of Adult T-cell Leukemia

Treatment of Adult T-cell Leukemia

Pathways of retinoic acid- or arsenic trioxide-induced PML/RARα catabolism, role of oncogene degradation in disease remission

Arsenic Trioxide Inhibits Human T Cell-Lymphotropic Virus-1-Induced Syncytiums by Down-Regulating gp46

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