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2898 Myelodysplastic Syndromes in Adolescent Young Adults (AYA)

Myelodysplastic Syndromes – Clinical Studies
Program: Oral and Poster Abstracts
Session: 637. Myelodysplastic Syndromes – Clinical Studies: Poster II
Sunday, December 6, 2015, 6:00 PM-8:00 PM
Hall A, Level 2 (Orange County Convention Center)

Joanna (Asia) Grabska, MD1, Bijal D. Shah, MD2, Najla H. Al Ali, BDS, MSc1*, Eric Padron, M.D.3, Hanadi Ramadan, BA1*, Jeffrey E Lancet, MD1, Alan F. List, MD4 and Rami S. Komrokji, MD5

1Malignant Hematology Department, H Lee Moffitt Cancer Center & Research Institute, Tampa, FL
2Department of Malignant Hematology, H. Lee Moffitt Cancer Center and Research Institute, Tampa, FL
3H Lee Moffitt Cancer Center & Research Institute, Tampa, FL
4Department of Hematologic Malignancies, Moffitt Cancer Center and Research Institute, Tampa, FL
5H. Lee Moffitt Cancer Center, Tampa, FL

Introduction:

There has been little improvement in cancer survival of adolescent and young adult (AYA) patients, ages 18-39, possibly reflecting different disease biology in this subgroup.  Myelodysplastic syndrome (MDS) is mainly a disease of the elderly.  The characteristics, outcomes and response to treatment are not well described among AYA population. 

Patients and Methods:

Retrospective review of patients from the Moffitt Cancer Center MDS database.  We compared baseline characteristics and outcomes of AYA population to older patients. Descriptive statistics were used for baseline characteristics. Chi-square test was used for categorical variables, and t-test for continuous variables comparison. Kaplan-Meier estimates were used for overall survival (OS), and cox regression method for multivariable analysis.

Results:

We identified 51 AYA and 1,897 older MDS patients.  Table-1 summarizes baseline characteristics.  More females and Hispanics were noted in AYA group.  The AYA patients had higher risk disease, more circulating myeloblasts and more hypoplastic MDS.  Autoimmune disorders were more prevalent in older patients.

The median OS was 47 months (mo) in the AYA group versus 40 mo in the older group (p 0.26).  The median OS was 47 mo versus 56 months in lower risk (low and intermediate-1(int-1)) IPSS MDS AYA group and older group respectively (p 0.46).  In the higher risk IPSS group (int-2 and high), median OS was 82 mo in AYA group compared to 17 mo in older group (p 0.001).  Thirty individuals were transplanted in the AYA versus 241 in the older group.  The median OS for transplanted patients was 55 mo in the AYA group and 46 mo in the older (p 0.4).  Whereas, in the non-transplanted patients median survival was 31 months for AYA and 39 months for the older group (p 0.9).  The rate of AML transformation was 37% versus 28% in AYA and older group respectively (p 0.17).  No difference in use or response to hypomethylating agents was observed.  Lenalidomide therapy was seldom used in younger patients.

In AYAs, poor karyotype was the only variable strongly associated with worse outcome. Fifteen patients had poor risk karyotype.  The median OS was 47 months, not reached and 29 months among patients with good, intermediate and poor risk cytogenetics, respectively (p 0.035)

Conclusion:

MDS is rare and tends to be more aggressive in the AYA population.  The karyotype was the most important prognostic factor. The differences in underlying disease biology should be further explored. Allogeneic stem cell transplant offered younger patients best outcomes.

Table 1: Baseline characteristics of AYA and Older Patient

Characteristic

AYA (18-39) (N= 51)

Older Patients (> 39 years old) (N=1,897)

P value

Gender

Female

25 (49%)

655 (34.5%)

0.025

Race

White

Black

Hispanic

Other

34 (66.7%)

2 (3.9%)

13 (25.5%)

2 (3.9%)

1,736 (91.5%)

47 (2.5%)

57 (3%)

41 (2.2%)

0.000

t-MDS

Yes

10 (19.6%)

359 (18.9%)

0.902

WHO Subtype

RA

RARS
RCMD

Deletion 5q

RAEB-1

RAEB-2

AML

CML

MDS-U

MDS/MPN

3 (5.9%)

1 (2%)

22 (43.1%)

0 (0%)

11 (21.6%)

10 (19.6%)

0 (0%)

0 (0%)

1 (2%)

2 (3.9%)

196 (10.4%)

151 (8%)

583 (30.8%)

51 (2.7%)

372 (19.7%)

336 (17.7%)

1 (0.1%)

60 (3.2%)

44 (2.3%)

94 (5%)

0.188

IPSS

Lower risk

Higher risk

28 (59.6%)

19 (40.4%)

1,264 (68.2%)

590 (31.8%)

IPSS-R

Very low/low

Intermediate

High/very high

13 (30.1%)

14 (32.6%)

16 (37.3%)

826 (45.3%)

394 (21.6%)

602 (33%)

Hypoplastic BM

Yes

11 (23.4%)

178 (9.8%)

0.009

LGL clone

Yes

0 (0%)

159 (8.4%)

0.033

Autoimmune disease

Yes

8 (15.7%)

500 (26.4%)

0.055

Karyotype

Good

Intermediate

Poor

24 (50%)

9 (18.8%)

15 (31.3%)

1120 (60.4%)

300 (16.2%)

434 (23.4%)

0.324

Peripheral Blasts

Yes

14 (29.8%)

246 (13.2%)

0.003

RBC Transfusion

Dependent

36 (70.6%)

1274 (67.3%)

0.372

 

Disclosures: Shah: Seattle Genetics: Research Funding ; Rosetta Genomics: Other: Grant support ; Acetylon: Other: Advisory board ; Plexus Communications: Honoraria ; Pharmacyclics: Speakers Bureau ; Spectrum: Other: Advisory board , Speakers Bureau ; Bayer: Honoraria ; Celgene: Other: Advisory board , Speakers Bureau ; DeBartolo Institute for personalized medicine: Other: Grant support . Lancet: Pfizer: Consultancy ; Kalo-Bios: Consultancy ; Boehringer-Ingelheim: Consultancy ; Amgen: Consultancy ; Seattle Genetics: Consultancy ; Celgene: Consultancy , Research Funding . List: Celgene Corporation: Honoraria , Research Funding . Komrokji: Celgene: Consultancy , Research Funding ; Incite: Consultancy ; Novartis: Speakers Bureau ; GSK: Research Funding .

*signifies non-member of ASH