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Blood, 15 February 2005, Vol. 105, No. 4, pp. 1837-1838. This Article Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Rights and Permissions Citing Articles Citing Articles via CrossRef Citing Articles via Google Scholar Google Scholar Articles by Wilson, J. L. Articles by Johansson, B. Search for Related Content PubMed PubMed Citation Articles by Wilson, J. L. Articles by Johansson, B. Related Collections Related Article in Blood Online Social Bookmarking                   What's this?  Previous Article  |  Table of Contents CORRESPONDENCE To the editor: No evidence for preferential maternal origin of duplicated chromosome 14 in hyperdiploid ALL Hyperdiploid childhood acute lymphoblastic leukemia (ALL) is associated with the nonrandom gain of chromosomes, most commonly X, 4, 6, 10, 14, 17, 18, and 21, and is thought to arise as a consequence of a single aberrant mitosis that then becomes clonal.1 Paulsson et al1 investigated the parental origin of trisomies in ALL hyperdiploid cases and found that in 7 of 8 cases with trisomy 14 (+14) the duplicated chromosome was of maternal origin. Previous research by our group2 has shown a preferential maternal loss of 9p21 alleles in 9 of 10 ALL cases, suggesting a possible role for epigenetic factors in the onset of ALL. Given that imprinting has been found in a number of genes on chromosome 143 and both maternal and paternal uniparental disomy of chromosome 14 have clinical phenotypes,4 Paulsson et al's1 observations warranted further investigation. We determined the parental origin of +14 in ALL cases held in our laboratory. Children with ALL were recruited at pediatric oncology clinics in New Zealand. DNA was extracted from presentation and remission bone marrow slides as published.2 Parental DNA was extracted from peripheral blood. Using diagnostic cytogenetic reports, 7 probable +14 ALL cases from children aged 23 months to 8 years were selected. In 5 cases +14 was specifically reported, while in 2 cases +14 was likely from the reported karyotype. Microsatellite markers D14S306 (14q21.1), D14S587 (14q22.2), and D14S617 (14q32.12) were examined. Samples were initially analyzed with D14S587, and then with other markers if the initial results were uninformative or ambiguous. The -P32 deoxycytidine triphosphate (dCTP)--labeled polymerase chain reaction (PCR) products were electrophoresed on 6% polyacrylamide sequencing gels, and the products visualized using a Fuji Bas-1500 phosphoimager (Fujifilm, Tokyo, Japan). Allele ratios were determined by dividing the size of the upper allele by the size of the lower allele. The leukemia DNA allele ratios were divided by remission ratios to standardize for bias due to preferential amplification of the shorter allele. Aratio of approximately 1 was interpreted as no trisomy, a ratio of 2 as duplication of the upper allele, while a ratio of 0.5 suggested duplication of the lower allele. The parental origin of the duplicated allele was determined visually. Of the 7 cases, 4 had paternal and 3 maternal inheritance of +14 (Table 1). In 2 cases the ratios were not as expected, but these do not alter the overall conclusion. Case 1710 showed disconcordant ratios for the 2 markers tested. The cytogenetic information for this case included del(?13), and if the deletion actually affected chromosome 14 then there would be partial tetrasomy, which might explain our result. There was insufficient DNA to analyze this sample at other markers. Case 1744 showed a 3:1 ratio at 2 markers suggesting the presence of 4 copies of chromosome 14, but the karyotype showed partial trisomy to 14q32. View this table: [in this window] [in a new window]   Table 1.. Karyotype, allele ratios, and parental origin of duplicated chromosome 14   Our results do not show any parental bias with respect to the duplication of chromosome 14. Although the possibility that imprinted genes are involved in childhood ALL is appealing, our data do not support the possible bias reported by Paulsson et al.1 Jackie L. Wilson, and Ian M. Morison Correspondence: Ian M. Morison, Cancer Genetics Laboratory, Department of Biochemistry, University of Otago, PO Box 56, Dunedin, New Zealand; e-mail: ian.morison{at}otago.ac.nz Footnotes Supported by the Health Research Council of New Zealand and the Cancer Society of New Zealand. References Paulsson K, Panagopoulos I, Knuutila S, et al. Formation of trisomies and their parental origin in hyperdiploid acute lymphoblastic leukemia. Blood. 2003;102: 3010-3015.[Abstract/Free Full Text] Morison IM, Ellis LM, Teague LR, Reeve AE. Preferential loss of maternal 9p in alleles childhood acute lymphoblastic leukemia. Blood. 2002;99: 375-377.[Abstract/Free Full Text] Morison IM, Paton CJ, Cleverly SD. The imprinted gene and parent-of-origin effect database. Nucleic Acids Res. 2001;29: 275-276.[Abstract/Free Full Text] Sutton VR, Shaffer LG. Search for imprinted regions on chromosome 14: comparison of maternal and paternal UPD cases with cases of chromosome 14 deletion. Am J Hum Genet. 2000;93: 381-387.   Response: The parental origin of trisomy 14 in hyperdiploid childhood ALL In a recent study,1 commented upon by Wilson and Morison, we investigated the formation of the hyperdiploid pattern in childhood acute lymphoblastic leukemia (ALL) and the possibility of imprinting effects related to the parental origin of the gained chromosomes,2,3 using a large set of polymorphic microsatellite markers. The finding of equal allele dosage for tetrasomy 21 indicated that hyperdiploidy most likely originates through a simultaneous gain of chromosomes in a single abnormal mitosis. Furthermore, no preferential duplications of maternal or paternal copies of chromosomes X, 4, 6, 10, 17, 18, and 21 were seen, and we concluded that imprinted regions on the duplicated chromosomes are generally not of major pathogenetic importance in hyperdiploid childhood ALL. However, 2 possible exceptions to the just-mentioned conclusion were noted. Trends toward significance were seen for trisomies 8 and 14: +8 was of paternal origin in 4 of 4 cases (P = .125) and +14 was of maternal origin in 7 of 8 cases (P = .0703)—findings that were noteworthy considering that imprinted regions have been shown to reside in at least the latter of these 2 chromosomes.4 Unfortunately, our limited number of cases precluded definitive conclusions.1 We now read with great interest the letter by Wilson and Morison, in which they report 7 cases of trisomy 14. Their results of 4 cases with paternal inheritance and 3 with maternal inheritance strongly indicate that the trend toward preferential maternal origin in our previous study does not represent a true skewness in the duplication process for chromosome 14. In fact, we have similar findings in an ongoing study of additional hyperdiploid childhood ALLs. Of 9 cases with trisomy 14, only 4 had maternal origin for the gained chromosome (P = .50; K.P. and B.J., unpublished data, December 15, 2004). Taken together, our previous study,1 the present results by Wilson and Morison, and our ongoing investigation strongly indicate that there is no preferential duplication of the maternal chromosome 14. Thus, imprinting effects related to the parental origin of trisomy 14 are most likely not of pathogenetic importance in hyperdiploid childhood ALL. Kajsa Paulsson, and Bertil Johansson Correspondence: Kajsa Paulsson, Department of Clinical Genetics, University Hospital, SE-221 85 Lund, Sweden; e-mail: kajsa.paulsson{at}klingen.lu.se. References Paulsson K, Panagopoulos I, Knuutila S, et al. Formation of trisomies and their parental origin in hyperdiploid childhood acute lymphoblastic leukemia. Blood. 2003;102: 3010-3015.[Abstract/Free Full Text] Onodera N, McCabe NR, Rubin CM. Formation of a hyperdiploid karyotype in childhood acute lymphoblastic leukemia. Blood. 1992;80: 203-208.[Abstract/Free Full Text] Haas OA. Is genomic imprinting involved in the pathogenesis of hyperdiploid and haploid acute lymphoblastic leukemia of childhood? Acta Genet Med Gemellol (Roma). 1996;45: 239-242.[Medline] [Order article via Infotrieve] Morison IM, Paton CJ, Cleverley SD. The imprinted gene and parent-of-origin effect database. Nucleic Acids Res. 2001;29: 275-276.[Abstract/Free Full Text] CiteULike    Connotea    Del.icio.us    Digg    Reddit    Technorati    What's this? Related Article in Blood Online: Formation of trisomies and their parental origin in hyperdiploid childhood acute lymphoblastic leukemia Kajsa Paulsson, Ioannis Panagopoulos, Sakari Knuutila, Kowan Ja Jee, Stanislaw Garwicz, Thoas Fioretos, Felix Mitelman, and Bertil Johansson Blood 2003 102: 3010-3015. [Abstract] [Full Text] [PDF] This Article Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Rights and Permissions Citing Articles Citing Articles via CrossRef Citing Articles via Google Scholar Google Scholar Articles by Wilson, J. L. Articles by Johansson, B. Search for Related Content PubMed PubMed Citation Articles by Wilson, J. L. Articles by Johansson, B. Related Collections Related Article in Blood Online Social Bookmarking                   What's this?

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