Cytogenetic studies of long‐term survivors of childhood acute lymphoblastic leukemia: A follow‐up report

Rubin, Charles M.; Robison, Leslie L.; Nesbit, Mark E.; Arthur, Diane C.

doi:10.1002/mpo.2950140602

Cited by 6 publications

(4 citation statements)

References 15 publications

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“…The most obvious of these is constitutional cytogenetics of survivors, with the idea that these would reflect mutations in germline chromosomes. The results of Rubin et al [29] suggest that this is not so; the majority of survivors of childhood ALL (who do not have abnormal children) harbor a small population of longlived lymphocytes that exhibit stable nonclonal chromosomal abnormalities. Survivors of pediatric cancer have been shown to have other markers of chromosomal injury in peripheral blood, such as sister chromatid exchanges, and mutations at the glycophorin A, HGPRT, and T-cell antigen receptor loci [30][31][32].…”

Section: Future Plansmentioning

confidence: 91%

Pregnancy outcome in long-term survivors of childhood cancer

Blatt

1999

Med. Pediatr. Oncol.

157

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Section: Future Plansmentioning

confidence: 91%

Pregnancy outcome in long-term survivors of childhood cancer

Blatt

1999

Med. Pediatr. Oncol.

157

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“…The persistence of stable aberrations in peripheral blood lymphocytes following radiation exposure has long been recognised by those studying the after effects of radiotherapy, although little has been done to quantify the frequencies in relation to the time course following exposure. A G-banding study of a group of survivors of childhood leukaemia (Rubin et al 1986) reported similar overall frequencies of chromosomally aberrant cells at 3.9 and 7.2 years post-exposure but the initial yield after treatment was not examined. A group of thyroid patients displayed similar raised frequencies of translocations 1 week and 3.5 years after treatment with radioactive iodine (Puerto et al 2000).…”

Section: Discussionmentioning

confidence: 99%

Persistence of translocation frequencies in blood lymphocytes following radiotherapy: implications for retrospective radiation biodosimetry

Tawn¹,

Whitehouse²

2003

J. Radiol. Prot.

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Chromosome aberration analysis using a G-banding technique was performed on peripheral blood lymphocyte cultures from eight individuals over a 5 year period following therapeutic radiation exposure. Samples were placed in three time periods comprising 0-12, 12-36 and 36-60 months post-treatment. The group was heterogeneous with respect to exposure and this resulted in wide differences in initial total translocation yields. Total translocation frequencies declined in seven of the eight cases, reaching significance in four cases. This decline was attributed to a decrease in cells, which in addition to translocations, also contained aberrations such as dicentrics which resulted in them being unstable. In all eight cases, when only stable cells were considered, no significant differences were observed in translocation frequencies between the different time periods post-treatment. Thus, although the frequency of translocations in stable cells is persistent over time, extrapolating to total initial yield, and using this to equate to dose, is not possible in cases where the exposure has been high and non-homogeneous. In practice, retrospective biological dosimetry is more often required in cases of historical, usually protracted, exposures which will have been essentially uniform and not of a sufficiently high dose for many cells to have acquired more than one aberration. In such cases the frequency of translocations observed some years after the exposure can be assumed to reflect induced frequencies and be used for dose estimation.

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“…Factors reported to be associated with secondary malignancies after bone marrow transplant include the presence of acute graft vs. host disease treated with either antithymocyte globulin or an anti-CD3 monoclonal antibody, T-lymphocyte depletion of the donor, HLA mismatch between donor and recipient, and use rearrangement in the causation of secondary malignancies posttransplant; however, consistent karyotypic changes have been observed in a growing number of human malignancies (Mitelman et al, 1990), including secondary neoplasms (Arthur and Bloomfield, 1984; Le Beau et al, 1986Ratain et al, 1987Pui et al, 1989Pui et al, , 1990Albain et al, 1990;Rubin et al, 1991). Given that cells with treatment-induced chromosome abnormalities can survive for long periods (Engel et al, 1964;Visfeldt, 1966Miller et al, 1978Savage and Bigger, 1978;Mouthuy and Dutrillaux, 1982;Robison et al, 1982;Rubin et al, 1986;Zaslav et al, 1988;Barrios et al, 1989), we speculate that certain of these cells with chromosome rearrangements involving critical genes are preneoplastic and may undergo subsequent genetic changes that result in malignant transformation.…”

Section: Discussionmentioning

confidence: 99%

“…Ionizing radiation and many chemotherapeutic drugs are mutagenic, with the capacity to produce detectable cytogenetic alterations, and are carcinogenic in a variety of in vitro and animal test systems. Exposure of man to certain of these agents is associated with the sustained presence of hematopoietic (Miller et al, 1978Robison et al, 1982Rubin et al, 1986;Barrios et al, 1989) and nonhematopoietic (Engel et al, 1964, Visfeldt, 1966Savage andBigger, 1978 Mouthuy andDutrillaux, 1982;Zaslav et al, 1988) cells with chromosomal abnormalities and an increased risk of secondary malignancies (reviewed by Holm, 1990). It is possible that development of secondary malignancy involves therapy-induced DNA damage in the form of gene mutation or chromosome alteration resulting in conversion of a normal cell into an initiated or preneoplastic one.…”

Section: Introductionmentioning

confidence: 99%

Chromosomal abnormalities in skin following total body or total lymphoid irradiation

Rubin

Nesbit

Kersey

et al. 1992

Genes Chromosomes & Cancer

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Patients undergoing bone marrow transplantation often receive total body or total lymphoid irradiation as part of the conditioning regimen prior to marrow infusion. The cytogenetic effects of this therapy on skin fibroblasts were studied. Fibroblast cultures from eight skin biopsies were harvested in early passages for G-banded chromosome analysis. Four biopsies were from three patients who had high-dose cyclophosphamide and total body radiotherapy; one was from within and one was from outside the radiation field of a patient who had high-dose cyclophosphamide and lymphoid radiotherapy, one was from a patient who had combination chemotherapy alone, and one was from a normal control. No abnormal mitoses were found in the control or the patient who had chemotherapy alone, and only two of 30 mitoses from skin outside the lymphoid radiotherapy field were abnormal. However, most cells (49-88%) from five biopsies within radiotherapy fields were abnormal. Typically, abnormal karyotypes were pseudodiploid and contained multiple balanced rearrangements, of which reciprocal translocations were most common. The data indicate that the radiotherapy used for bone marrow transplantation induces extensive, sustained chromosome abnormalities in vivo in skin fibroblasts.

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Cytogenetic studies of long‐term survivors of childhood acute lymphoblastic leukemia: A follow‐up report

Cited by 6 publications

References 15 publications

Pregnancy outcome in long-term survivors of childhood cancer

Pregnancy outcome in long-term survivors of childhood cancer

Persistence of translocation frequencies in blood lymphocytes following radiotherapy: implications for retrospective radiation biodosimetry

Chromosomal abnormalities in skin following total body or total lymphoid irradiation

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