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Journal ArticleDOI

Polyclonal integration of HTLV-I proviral DNA in lymphocytes from HTLV-I seropositive individuals : An intermediate state between the healthy carrier state and smouldering ATL

TLDR
The only haematological abnormality in these patients was the presence of few atypical lymphoid cells in the peripheral blood.
Abstract
Summary We have studied 15 individuals (aged 14-74 years) with antibodies to HTLV-I in their serum and random integration of HTLV-I proviral DNA in their peripheral blood lymphocytes. All but one of these patients suffered from a variety of non-specific complaints which did not correspond to those of adult T-cell leukaemia (ATL). All of them were born in Kyushu and Okinawa which are endemic areas for HTLV-I infection; 25% of their family members were also seropositive for HTLV-I. The only haematological abnormality in these patients was the presence of few atypical lymphoid cells in the peripheral blood. The CD4/CD8 ratios were normal but the proportion of Tac positive cells was slightly higher than normal. These individuals with polyclonal integration of HTLV-I proviral DNA seem to represent an intermediate state between smouldering ATL (monoclonal integration) and healthy HTLV-I carriers (with antibodies but no detectable HTLV-I proviral DNA). Patients with this intermediate state of HTLV-I infection may be at risk to progress to ATL. The natural history of HTLV-I infection in humans leading to the development of ATL is reviewed in the light of these new findings.

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Diagnostic criteria and classification of clinical subtypes of adult T-cell leukaemia-lymphoma. A report from the Lymphoma Study Group (1984-87).

TL;DR: The following diagnostic criteria are proposed to classify four clinical subtypes of HTLV‐1 associated adult T‐cell leukaemia‐lymphoma (ATL): smouldering type, 5% or more abnormal lymphocytes of T‐ cell nature in PB, normal lymphocyte level, no hypercalcaemia, and histologically‐proven lymphadenopathy and involvement of liver, spleen, skin, and lung.
Journal ArticleDOI

Two types of defective human T-lymphotropic virus type I provirus in adult T-cell leukemia

TL;DR: The high frequency of this defective virus in the aggressive form of ATL suggests that it may be caused by the genetic instability of HTLV-I provirus, and cells with this defectiveirus are selected because they escape from immune surveillance systems.
Journal ArticleDOI

Adult T-Cell Leukemia: A Review of Epidemiological Evidence

TL;DR: The current epidemiological evidence is insufficient to fully understand the oncogenesis of ATL, and further well-designed epidemiological studies are needed.
Journal Article

Persistent Clonal Proliferation of Human T-lymphotropic Virus Type I-infected Cells in Vivo

TL;DR: Findings indicate that HTLV-I infection plays an important role in the clonal expansion of lymphocytes and the prolonged survival of CD4-positive cells in vivo, and may be susceptible to genetic changes, leading to the onset of leukemia.
References
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Journal ArticleDOI

Detection and isolation of type C retrovirus particles from fresh and cultured lymphocytes of a patient with cutaneous T-cell lymphoma

TL;DR: The number of these particle-associated proteins is consistent with the expected proteins of a retrovirus, but the sizes of some are distinct from those of most known retroviruses of the primate subgroups.
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Adult T-cell leukemia : antigen in an ATL cell line and detection of antibodies to the antigen in human sera

TL;DR: Antibodies against the antigen in MT-1 cells were found in all 44 patients with ATL examined and in 32 of 40 patients with malignant T-cell lymphomas (most of them had diseases similar to ATL except that leukemic cells were not found in the peripheral blood).
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Isolation and characterization of retrovirus from cell lines of human adult T-cell leukemia and its implication in the disease

TL;DR: Findings on the close association of ATLV protein and proviral DNA with ATL are direct evidence for the possible involvement of the retrovirus ATLV in leukemogenesis of human ATL.
Journal ArticleDOI

Adult T-cell leukemia: clinical and hematologic features of 16 cases

TL;DR: In this paper, clinical and hematologic studies of 16 adult patients whose leukemic cells had T-cell markers are reported from Japan, where the incidence of various lymphoproliferative diseases differs considerably from that in Western countries.
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Human c-myc onc gene is located on the region of chromosome 8 that is translocated in Burkitt lymphoma cells

TL;DR: Using a DNA probe that is specific for the complete gene (c-myc), different somatic cell hybrids possessing varying numbers of human chromosomes were analyzed by the Southern blotting technique and results indicate that the human c- myc gene is located on chromosome 8.
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