Paper #23205 A Methylation Profile of Tumor Suppressor Genes

Transcripción

Paper #23205
A Methylation Profile of Tumor Suppressor Genes
Predicts a Poorer Survival in Patients with
Refractory Anemia with Ringed Sideroblasts
Ana Valencia1*, Jose Cervera1*, Esperanza Such1*, Esther Gamero1*, Mariam
Ibañez1*, Silvestre Oltra2*, Maria Leonor Senent1*, Amparo Sempere1*, Federico
Gomis1*, Maria Luz Perez-Sirvent1*, Miguel Sanz, MD, PhD1* and Guillermo Sanz,
MD, PhD1
1
Department of Hematology, Hospital Universitario La Fe, Valencia, Spain; 2Genetic
Unit, Hospital Universitario La Fe, Valencia, Spain
Patients with refractory anemia with ring sideroblasts (RARS) are considered to
have good prognosis and anemia is usually managed with best supportive care and
erythroid stimulating agents. Nowadays, no specific molecular marker related to
outcome and disease progression has been identified. Several genes involved in
cell cycle and apoptosis that may become inactivated by aberrant hypermethylation
have been identified in patients with myelodysplastic syndromes (MDS) but the
significance of a methylation profile (studying several genes at the same time) in
RARS is unknown, mainly because the number of patients with RARS in published
reports is rather low. To assess the implication of aberrant methylation in RARS, we
studied the methylation status of 25 sequences of a set of tumor suppressor genes
in 40 patients (median age 70 yr, 25 male gender) with RARS according to FAB
criteria [WHO classification, RARS in 22 patients (55%); refractory citopenia with
multilineage dysplasia and ring sideroblasts, 18 (45%)] by means of methylationspecific multiplex ligation-dependent probe amplification (MS-MLPA) assay. The
MS-MLPA procedure (SALSA MLPA kit ME001, MRC-Holland, Amsterdam, The
Netherlands) has been developed for detecting in a semi-quantitative manner
changes in the methylation status of 25 tumor suppressor genes in a single
experiment. Briefly, approximately 50 ng of DNA were denatured and hybridized
with MLPA probes. Subsequently, the probes were ligated in half of every sample,
whereas for the rest of the sample, ligation was combined with an endonuclease
HhaI digestion resulting in ligation of the methylated sequences only. PCR was
performed as described by the manufacturer, and then separated by capillary gel
electrophoresis and quantified using the Genemapper software (ABI 310, Applied
Biosystems, Foster City, CA). Quantification of the methylation status was done by
dividing the peak area with the combined areas of the control probes lacking the
target sequence of the HhaI. Finally, the relative peak area of each target probe
from the digested sample was compared with those obtained from the undigested
sample. Aberrant methylation was scored when the calculated methylation
percentage was >10%. To validate the MS-MLPA method the methylation status of
CDKN2B was also analyzed by methylation-specific PCR (MSP). Actuarial curves of
OS were built by Kaplan-Meier method and differences between curves compared
with log-rank tests. Small numbers precluded the use of multivariate methodology.
The MS-MLPA analysis detected methylation of at least one gene in 17 patients
(42.5%). The genes aberrantly methylated were CDKN2B (n = 8, 20%), RASSF1 (n
= 7, 17%), RARB (n = 3, 7.5%), CDH13 (n = 3, 7.5%) and FHIT (n = 2; 5%). Of the
17 patients, five (12%) presented methylation in two genes (RASSF1-FHIT in 2,
RASSF1-RARB in 1, RASSF1-CDH13 in 1, and CDKN2B-CDH13 in 1, who was the
only patient who progressed to AML). The presence of aberrant gene methylation
was not significantly associated with any clinical or biological characteristic or WHO
morphological subtype. Patients with aberrant gene methylation had a significantly
shorter overall survival (OS) than patients without methylated genes (median OS,
72 mo vs 114 mo, respectively; P = 0.03). Patients with hemoglobin level below 10
g/dL and platelet count below 150 ×109/L also had a significantly poorer OS (P=
0.01 and P= 0.02, respectively). As the majority of probes used in the MS-MPLA
method detect methylation in only one CpG pair, the results of CDKN2B methylation
were validated by MSP, which yielded the same methylation results than with MSMPLA methodology. The 8 patients with methylated CDKN2B show a trend for a
shorter survival than the remaining 32 with unmethylated CDKN2B (median 72 mo
vs 114 mo, P = 0.08). The results of this study indicate that aberrant methylation of
several tumor suppressor genes is observed in a substantial proportion of patients
with RARS. As occurs in patients with high-risk MDS, our results suggest that
aberrant gene methylation confers a poor prognosis in RARS, but these data and
their potential independent value require confirmation in larger series that employ
multivariate methods. Finally, these findings provide a strong rationale for the use of
hypomethylating agents (e.g., azacitidine or decitabine) in patients with RARS.
This work has been partially supported by ISCIII grants RD06/0020/0031 and
CA08/00141.
Title: A Methylation Profile of Tumor Suppressor Genes Predicts a Poorer Survival
in Patients with Refractory Anemia with Ringed Sideroblasts
Review Category Selection: 633. Myelodysplastic Syndromes
Preferred Presentation Format: Oral
Submitter's E-mail Address: [email protected]
Publish only on the Blood Abstracts site: Yes
First submission to an ASH Annual Meeting: Yes
Compliance with the Declaration of Helsinki for Studies Involving Human
Subjects: Agree
Is the first author/presenter of this abstract a hematologist in training?: No
Interim Analysis of Clinical Trial: No
Special Consideration: No
Hematologist in training: No
Keywords: MDS, Methylation
First Author
Presenter
Corresponding
Ana Valencia
Department of Hematology
Hospital Universitario La Fe
Valencia,
Spain
Phone Number: 0034961973057
Fax Number: 0034961973281
Email: [email protected]
I have relevant financial relationship(s) to disclose. No
My presentation and/or paper will include information or discussion of offlabel drug use. No
Signed on 08/18/2009 by Ana Valencia
Second Author
Jose Cervera
Avenida Campanar 21
Valencia,
Spain
Phone Number: 34 (963) 862709
Fax Number: 34 (961) 973280
Email: [email protected] -- Will not be published
Signed on 08/18/2009 by Jose Cervera
Third Author
Esperanza Such
Valencia,
Spain
Email: [email protected]
Signed on 08/18/2009 by Esperanza Such
Fourth Author
Esther Gamero
Valencia, 46009
Spain
Fax Number: 0034961973281
Signed on 08/18/2009 by Esther Gamero
Fifth Author
Mariam Ibañez
Valencia, 46009
Spain
Fax Number: 0034961973281
Signed on 08/18/2009 by Mariam Ibañez
Sixth Author
Silvestre Oltra
Genetic Unit
Avda Campanar 21
Valencia, 46009
Spain
Fax Number: 00349601973281
My presentation and/or paper will include information or discussion of off-
label drug use. No
Signed on 08/18/2009 by Silvestre Oltra
Seventh Author
Maria Leonor Senent
Avenida Campanar 21
Valencia, 46009
Spain
Fax Number: 0034961973051
Signed on 08/18/2009 by Maria Leonor Senent
Eighth Author
Amparo Sempere
Avenida Campanar 21
Valencia, 46009
Spain
Fax Number: 0034961973251
Signed on 08/18/2009 by Amparo Sempere
Ninth Author
Federico Gomis
Avenida Campanar 21
Valencia, 46009
Spain
Fax Number: 0034961973157
Signed on 08/18/2009 by Federico Gomis
Tenth Author
Maria Luz Perez-Sirvent
Avenida Campanar 21
Valencia, 46009
Spain
Fax Number: 0034961973281
Signed on 08/18/2009 by Maria Luz Perez_Sirvent
Eleventh Author
Miguel Sanz, MD, PhD
Valencia,
Spain
Signed on 08/18/2009 by Miguel Sanz
Twelfth Author
Guillermo Sanz, MD, PhD
Avenida Campanar 21
Valencia, 46009
Spain
Phone Number: 34 (963) 862709
Fax Number: 34 (961) 973280
Signed on 08/18/2009 by Guillermo Sanz

Paper #23205 A Methylation Profile of Tumor Suppressor Genes

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