Complex variant 9;22 translocations occur in a significant minority of chronic myelogenous leukaemia (CML) patients. Different mechanisms of their formation have been described. We report dual colour dual fusion fluorescence in situ hybridisation data in 12 Chinese CML patients with complex translocations. Three previously reported breakpoint hotspots in a third partner chromosome (14q32, 17q25, 1q2l) were observed. In 10/12 (83.3%) patients, the abnormality occurred as a single step 3-break event. Only a single abnormal clone harbouring the complex translocation was seen in this group. The remaining 2 cases in the chronic phase showed a 4-break mechanism (2/12,16.7%). Deletion of 5' ABL at der(9) was not observed in any of the 12 patients, however, the loss of 3' BCR was observed in 1 patient (1/12, 8.3%). Together with previous findings, these data suggest that these variant translocations occur more often as a 3-break single-step process with no reciprocal ABL-BCR fusion. On the other hand, a 4-break event is also regularly seen during the initial stages of leukaemogenesis, which likely predisposes to der(9) deletion. The observed difference in rates of der(9) deletion reported in a series of CML patients with variant translocations may be related to a difference in rates of a 4-break event.published_or_final_versio

Chan, LC

So, CC

Wan, TSK

Yip, SF

Oncology Reports

HKU Scholars Hub

TitleA dual colour dual fusion fluorescence in situ hybridisationstudy on the genesis of complex variant translocations inchronic myelogenous leukaemiaAuthor(s) So, CC; Wan, TSK; Yip, SF; Chan, LCCitation Oncology Reports, 2008, v. 19 n. 5, p. 1181-1184Issued Date 2008URL http://hdl.handle.net/10722/88783Rights Creative Commons: Attribution 3.0 Hong Kong LicenseAbstract. Complex variant 9;22 translocations occur in asignificant minority of chronic myelogenous leukaemia (CML)patients. Different mechanisms of their formation have beendescribed. We report dual colour dual fusion fluorescencein situ hybridisation data in 12 Chinese CML patients withcomplex translocations. Three previously reported breakpointhotspots in a third partner chromosome (14q32, 17q25, 1q21)were observed. In 10/12 (83.3%) patients, the abnormalityoccurred as a single step 3-break event. Only a singleabnormal clone harbouring the complex translocation wasseen in this group. The remaining 2 cases in the chronic phaseshowed a 4-break mechanism (2/12, 16.7%). Deletion of 5' ABLat der(9) was not observed in any of the 12 patients, however,the loss of 3' BCR was observed in 1 patient (1/12, 8.3%).Together with previous findings, these data suggest that thesevariant translocations occur more often as a 3-break single-step process with no reciprocal ABL-BCR fusion. On theother hand, a 4-break event is also regularly seen during theinitial stages of leukaemogenesis, which likely predisposes toder(9) deletion. The observed difference in rates of der(9)deletion reported in a series of CML patients with varianttranslocations may be related to a difference in rates of a4-break event.IntroductionComplex variant translocation of (9;22) has an incidence of~10% in patients with chronic myelogenous leukaemia (CML)(1,2). The most common is a 3-way balanced t(9;22;v).Previous studies using a chromosome 22 painting probeindicated either a one-step (3) or two-step process (4) in thegenesis of these variants. Recent studies using the fluorescencein situ hybridisation (FISH) method showed the occurrenceof either mechanism in different and occasionally the samecases (5,6).Chronic myelogenous leukaemia with der(9) deletion hasbeen shown to carry a poor prognosis (7-10). Complex varianttranslocations in CML have been reported in many studies tobe associated with a significantly higher incidence of der(9)deletion than CML with classical Ph translocation (weightedaverage 40.4 vs 12.7%) (reviewed in ref. 6). These trans-locations impart a poor survival to this group of patientswhen compared to CML patients with classical t(9;22) orvariant translocations without der(9) deletion (5).In this study, we employed D-FISH to investigate themechanism of formation of the most common 3-way t(9;22;v)in 12 Chinese patients with CML. The incidence of der(9)deletion was also determined in this cohort of patients.Materials and methodsClinical samples. A search for complex variant translocationin CML patients was performed in our cytogenetics database.Twelve cases were identified which had available materialsfor D-FISH analysis - 10 in the chronic phase and 2 in theaccelerated phase. All showed a balanced 3-way t(9;22;v).Conventional cytogenetic analysis. Cytogenetic analysis wasperformed on Giemsa banded (G banded) metaphases obtainedthrough short-term synchronised and unsynchronised culturesof bone marrow cells based on standardised protocols.Karyotypes were reported in accordance with ISCN 1995.D-FISH. Detection of BCR-ABL and ABL-BCR gene fusionswas performed using BCR/ABL dual colour dual fusiontranslocation probes (Abbott Molecular/Vysis, Des Plaines,IL), according to the manufacturer's instructions. In total, 300interphase nuclei on cytospin smears were analysed for thepresence of fusion signals. In selected cases, metaphase FISHwas performed on G banded metaphases relocated usingmicroscope coordinates, as described previously (11). A2G2O1F pattern indicated a one-step 3-break event whereas a1G1O2F pattern indicated a two-step 4-break event.ResultsTable I shows the disease status during the investigationand full karyotype of the 12 cases with balanced 3-wayONCOLOGY REPORTS  19:  1181-1184,  2008A dual colour dual fusion fluorescence in situ hybridisation study on the genesis of complex variant translocations in chronic myelogenous leukaemia CHI-CHIU SO,  THOMAS SHEK-KONG WAN,  SZE-FAI YIP  and LI-CHONG CHANDepartment of Pathology, Li Ka Shing Faculty of Medicine, The University of Hong Kong, Hong Kong, P.R. ChinaReceived August 31, 2007;  Accepted October 22, 2007_________________________________________Correspondence to: Dr Chi-Chiu So, Department of Pathology,Li Ka Shing Faculty of Medicine, The University of Hong Kong,Hong Kong, P.R. ChinaE-mail: scc@pathology.hku.hkKey words: variant, cytogenetics, chronic myelogenous leukaemia,9q34 deletion, Chinese1181-1184  4/4/08  17:12  Page 1181translocations. Ten patients were in the chronic phase and 2in the accelerated phase. No patient was in the blast phase.None of them had received tyrosine kinase inhibitor therapyprior to investigation. Residual normal metaphases weredetected in only 1 case by conventional cytogenetics.Recurrent breakpoints in a third partner chromosome wereobserved at 5q11.2 (n=2) and 10p14 (n=2). Clonal evolutionwas evident in 2 cases. Case 9 showed a subclone withadditional trisomy 8 at disease acceleration. Case 12harboured a stem line with classical t(9;22), which was notseen in any other case in this series.In 10 cases, D-FISH revealed (8 chronic and 2 in theaccelerated phase) a 2G2O1F pattern indicating a one-step3-break event. A reciprocal ABL-BCR fusion signal wasabsent. Normal cells with a 2G2O pattern were observed in 3of these 10 cases in significant proportions (8-22%) ofinterphase nuclei examined. In the remaining 2 cases of thechronic phase CML, a 1G1O2F pattern was seen indicating atwo-step 4-break mechanism. This included the only case(Case 12) showing a stemline with classical t(9;22) andanother case (Case 11) with a single abnormal clone of varianttranslocation. Metaphase FISH analysis of these 2 casesshowed the presence of a fusion signal on der(9), indicating anintact ABL-BCR fusion gene and a further break distal to theABL breakpoint in the 3-way translocation (Fig. 1a, b and c).None of the 12 cases showed a loss of the 5' ABL signal onder(9), however, the loss of the 3' BCR signal on der(9) wasobserved in a subclone in 1 case (Case 11). The rate of der(9)deletion was thus 1/12 (8.3%).DiscussionIn CML, the most common form of complex variant trans-locations is 3-way balanced t(9;22;v). Indirect evidencesuggests a one-step process in the formation of these varianttranslocations in most incidences: i) They are usually observedat initial diagnosis of the chronic phase, although are notnormally detected as new cytogenetic abnormalities duringdisease evolution. ii) By themselves they do not signifydisease acceleration. iii) These variants are most often foundin the absence of a clone bearing classical t(9;22).The availability of D-FISH provides a useful tool ininvestigating the mechanism of the formation of these varianttranslocations in CML. Using this technique, a 3-break process(2G2O1F) and a 4-break two-step process (1G1O2F) haveboth been observed. The expected predominance of a 3-breakprocess was confirmed, which accounted for ~50% of the casesin recent large series (5,6). However, a significant minorityof cases with a 4-break two-step process was regularly seen(1,5,6). The incidence ranged from 6 to 21.4%. The sameobservation was also evident in the present study (2/12,16.7%). As expected, a 4-break process was detected in casesshowing a classical t(9;22) stemline (as Case 12 in the presentstudy). Notably, it was also found in patients with a singleabnormal clone showing variant translocation (as Case 11 inthe present study). This suggests that a 4-break mechanism canalso operate at the initial stages of leukaemogenesis, either asa one-step 4-break process or with a second translocationbetween der(9)t(9;22) and a third partner chromosomeoccurring shortly after t(9;22) in the same leukaemic stemcell. These 2 scenarios are expected to be rare compared to asimpler 3-break process. Therefore, the resulting 4-break D-FISH pattern was less commonly observed in most series. Werecently reported a similar case of the unusual 4-break processin a patient with acute promyelocytic leukaemia and a singleabnormal clone of 47,XY,+8,t(15;17;7)(q22;q12;q22) (12).A major difficulty is seen when D-FISH is employed tostudy how variant translocations arise in CML. It is notSO et al:  COMPLEX VARIANT TRANSLOCATION IN CML1182Table I. Disease status, full karyotype and D-FISH results.–––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––Case No. Disease phase Karyotype D-FISH patterna Interpretation–––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––1 Chronic 46,XY,t(5;9;22)(q31;q34;q11.2)[13] 89% 2G2O1F 3-break11% 2G2O Residual normal cells2 Chronic 46,XY,t(5;9;22)(q31;q34;q11.2)[7]/46,XY[1] 78% 2G2O1F 3-break22% 2G2O Residual normal cells3 Chronic 46,XX,t(9;22;10)(q34;q11.2;p14)[9] 100% 2G2O1F 3-break4 Chronic 46,XX,t(9;22;10)(q34;q11.2;p14)[6] 100% 2G2O1F 3-break5 Chronic 46,XY,t(9;22;14)(q34;q11.2;q32.1)[12] 100% 2G2O1F 3-break6 Chronic 46,XX,t(5;9;22)(p15;q34;q11.2)[10] 100% 2G2O1F 3-break7 Chronic 46,XY,t(9;22;17)(q34;q11.2;q25)[16] 100% 2G2O1F 3-break8 Chronic 46,XY,t(7;9;22)(q35;q34;q11.2)[8] 100% 2G2O1F 3-break9 Accelerated 46,XY,t(9;22;19)(q34;q11.2;q12.3)[5]/47,idem,+8[3] 100% 2G2O1F 3-break10 Accelerated 46,XX,t(1;9;22)(q21;q34;q11.2)[8] 92% 2G2O1F 3-break8% 2G2O Residual normal cells11 Chronic 46,XX,t(4;9;22)(p11;q34;q11.2)[16] 19% 1G1O2F 4-break81% 1G2O1F Loss of 3' BCR in subclone12 Chronic 46,XX,t(9;22)(q34;q11.2)[2] 100% 1G1O2F 2-break in stemline/46,XX,t(9;22;14)(q34;q11.2;q24)[9] 4-break in subclone–––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––aD-FISH pattern: G, green (BCR, 22q11.2); O, orange (ABL, 9q34); F, fusion (BCR-ABL; ABL-BCR).–––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––––1181-1184  4/4/08  17:12  Page 1182applicable to cases with der(9) deletion as one cannot deducewhether a 3-break or 4-break process has occurred before thedeletion. This has been an important confounding factor asder(9) deletion was observed in an average of 40% of cases inmost reported series (6). In the largest series reported todate, Reid et al (5) detected a frequency of 3-break and 4-break process in 52 and 11% of 54 patients with varianttranslocation, respectively. However, a significant 37% ofthe patients showed a der(9) deletion by D-FISH and thus atranslocation mechanism could not be assigned. As proposedby Huntly et al (9), each recombination at der(9q34) shouldhave a finite probability leading to deletion around the region.It is therefore reasonable to postulate that many, if not themajority, of those cases with der(9) deletion had a 4-breaktranslocation. This would be in agreement with the finding thatin series with a low frequency of der(9) deletion (1) includingthe present one, a much higher rate of 3-break events was seen(83 to 94%). The suggestion that a 4-break mechanism canalso operate at the initial stages of leukaemogenesis and thuspredisposes to deletion, as discussed above, is also consistentwith the many evidences favouring a 9q deletion eventoccurring at the time of formation of the Ph translocation (13).The reason for the possible difference in rates of a 4-breakevent among different series that might have explained theobserved variation in frequency of der(9) deletion is notapparent. An ethnic genetic difference cannot be excluded. Asimilar low rate of der(9) deletion (13.7%) was also reported ina cohort of Chinese CML patients with variant translocations(14). However, the rate of a 4-break event was not shown.Three reported breakpoint hotspots in a third partnerchromosome (14q32, 17q25, 1q21) (2) were observed in ourcases. In addition, 2 cases each with breakpoint at 5q31 and10p13 were found, which have not been found previously asbreakpoint hotspots. These breakpoint hotspots are locatedpreferentially in the GC-richest regions of the genome. GC-rich regions have high densities of genes and repetitive Alusequences. They also coincide with open chromatin with hightranscription activities. These elements may increase thechance of chromosome breakage and repair or the juxta-positioning of Alu-rich sites, resulting in chromosomalrecombination and translocation (2).In conclusion, complex variant translocation in CMLoccurs more often as a 3-break single-step process with noreciprocal ABL-BCR fusion. On the other hand, a 4-breakevent is also regularly observed during the initial stages ofleukaemogenesis. Although by itself it may not have aONCOLOGY REPORTS  19:  1181-1184,  2008 1183Figure 1. Aypical D-FISH pattern in Case 12. (a) Complete karyotype showing 46,XX,t(9;22;14)(q34;q11.2;q24). (b) D-FISH analysis on a relocated G bandedmetaphase with 1G1O2F. An ABL-BCR fusion signal is detected on der(9) (arrow), indicating a second break at 9q34 telomeric to the ABL breakpoint. Nosignal is seen on der(14) (arrowhead).1181-1184  4/4/08  17:12  Page 1183prognostic implication, a 4-break process likely predisposes toder(9) deletion which is a strong predictor of survival. Theobserved low frequency of der(9) deletion among ChineseCML patients with variant translocations can be due to a lowrate of a 4-break event. Further studies confirming andexplaining this difference are warranted in order to have abetter understanding of the pathogenesis of CML.References1. Aoun P, Wiggins M, Pickering D, Foran J, Rasheed H,Pavletic, SZ and Sanger W: Interphase fluorescence in situhybridization studies for the detection of 9q34 deletions inchronic myelogenous leukemia: a practical approach to clinicaldiagnosis. Cancer Genet Cytogenet 154: 138-143, 2004.2. Fisher AM, Strike P, Scott C and Moorman AV: Breakpoints ofvariant 9;22 translocations in chronic myeloid leukemia locatepreferentially in the CG-richest regions of the genome. GenesChromosomes Cancer 43: 383-389, 2005.3. Yehuda O, Abeliovich D, Ben-Neriah S, Sverdlin I, Cohen R,Varadi G, Orr R, Ashkenazi YJ, Heyd J, Lugassy G andBen Yehuda D: Clinical implications of fluorescence in situhybridization analysis in 13 chronic myeloid leukemia cases:Ph-negative and variant Ph-positive. Cancer Genet Cytogenet114: 100-107, 1999.4. Calabrese G, Stuppia L, Franchi PG, Peila R, Morizio E,Liberati AM, Spadano A, Di Lorenzo R, Donti E, Antonucci Aand Palka G: Complex translocations of the Ph chromosome andPh negative CML arise from similar mechanisms, as evidencedby FISH analysis. Cancer Genet Cytogenet 78: 153-159, 1994.5. Reid AG, Huntly BJ, Grace C, Green AR and Nacheva EP:Survival implications of molecular heterogeneity in variantPhiladelphia-positive chronic myeloid leukaemia. Br J Haematol121: 419-427, 2003.6. Gorusu M, Benn P, Li Z and Fang M: On the genesis andprognosis of variant translocations in chronic myeloid leukemia.Cancer Genet Cytogenet 173: 97-106, 2007.7. Sinclair PB, Nacheva EP, Leversha M, Telford N, Chang J,Reid A Bench A, Champion K, Huntly B and Green AR: Largedeletions at the t(9;22) breakpoint are common and may identifya poor-prognosis subgroup of patients with chronic myeloidleukemia. Blood 95: 738-743, 2000.8. Cohen N, Rozenfeld-Granot G, Hardan I, Brok-Simoni F,Amariglio N, Rechavi G and Trakhtenbrot L: Subgroup ofpatients with Philadelphia-positive chronic myelogenousleukemia characterised by a deletion of 9q proximal to ABLgene: expression profiling, resistance to interferon therapy, andpoor prognosis. Cancer Genet Cytogenet 128: 114-119, 2001.9. Huntly BJ, Reid AG, Bench AJ, Campbell LJ, Telford N,Shepherd P, Szer J, Prince HM, Turner P, Grace C, Nacheva EPand Green AR: Deletions of the derivative chromosome 9 occurat the time of the Philadelphia translocation and provide apowerful and independent prognostic indicator in chronicmyeloid leukemia. Blood 98: 1732-1738, 2001.10. Kolomietz E, Al-Maghrabi J, Brennan S, Karaskova J, Minkin S,Lipton J and Squire JA: Primary chromosomal rearrangements ofleukemia are frequently accompanied by extensivesubmicroscopic deletions and may lead to altered prognosis.Blood 97: 3581-3588, 2001.11. Wan TS, Ma SK, Ho MY, Chan LC, Yip SF, Wong LG andYeung YM: Cytogenetic biclonality in polycythemia vera:unusual and unrelated clones. Cancer Genet Cytogenet 131:86-89, 2001.12. Wan TS, So CC, Hui KC, Yip SF, Ma ES and Chan LC:Diagnostic utility of dual fusion PML/RARalpha translocationDNA probe (D-FISH) in acute promyelocytic leukemia. OncolRep 17: 799-805, 2007.13. Reid AG and Nacheva EP: Genesis of derivative chromosome 9deletions in chronic myeloid leukemia. Genes ChromosomesCancer 43: 223-224, 2005.14. Wu W, Xue YQ, Wu YF, Pan JL and Shen J: Study of deletion ofderivative chromosome 9 in patients with Ph+ chronic myeloidleukemia. Zhonghua Xue Ye Xue Za Zhi 27: 183-186, 2006.SO et al:  COMPLEX VARIANT TRANSLOCATION IN CML11841181-1184  4/4/08  17:12  Page 1184

A dual colour dual fusion fluorescence in situ hybridisation study on the genesis of complex variant translocations in chronic myelogenous leukaemia

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A dual colour dual fusion fluorescence in situ hybridisation study on the genesis of complex variant translocations in chronic myelogenous leukaemia

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