Elevated expression of the leukaemia associated antigen SSX2IP predicts good survival in acute myeloid leukaemia patients who lack detectable cytogenetic rearrangements
Elevated expression of the leukaemia associated antigen SSX2IP predicts good survival in acute myeloid leukaemia patients who lack detectable cytogenetic rearrangements
Greiner et al have previously described a positive association between elevated leukemia-associated antigen (LAA) expression (RHAMM, G250/CA9, and PRAME) and survival in 116 acute myeloid leukemia (AML) patients by microarray. We have analyzed 312 presentation AML samples using 199 133A chips and 113 Plus2 chips and segregated AML patients based on above- and below-median levels of expression of the LAA synovial sarcoma X breakpoint 2–interacting protein (SSX2IP). Analysis of Kaplan-Meier curves showed an association between elevated SSX2IP expression and improved survival times (log-rank test, P = .05). We found that SSX2IP expression did not predict the survival of AML patients who had detectable cytogenetic abnormalities; however, it was significantly associated with improved survival rates in patients with no detectable cytogenetic rearrangements (log-rank test, n = 180; P = .007). We also found a correlation between elevated SSX2IP expression and other clinical parameters that are considered to be good prognostic markers: days in remission (log-rank test, P = .03), age at diagnosis (< 60 years; t test, P = .003), and FLT3 WT (t test, P = .004). When we examined SSX2IP together with the expression of other LAAs known to be associated with improved survival, we found a significant correlation with SURVIVIN (Pearson correlation, P = 3.97 x 10–5) and RHAMM (Pearson correlation, P = 4.3 x 10–5). Other groups suggested that the expression of distinct LAAs on leukemic blasts may lead to the eradication of residual disease after intensive chemotherapy. RHAMM and Survivin, like SSX2IP, have increased expression in proliferating cells while RHAMM and SSX2IP are both expressed on the surface of malignant cells. There appears to be a small but growing group of LAAs that are coexpressed in AML patients and are associated with improved survival. We examined whether having 1 or more of SSX2IP, Survivin, or RHAMM affected survival in patients with a normal karyotype and found that having expression of none, 1, 2 or all 3 of these LAAs was a significant prognostic indicator (log-rank test, P = .021, respectively). With regard to the presence of cytogenetic abnormalities, these appear to supersede the influence of elevated LAA expression on prognosis.
In summary, we have found that SSX2IP expression at disease presentation predicts good survival in AML patients with no detectable cytogenetic rearrangements. This may, in part, explain why patients with low LAA expression (often the elderly) fail to elicit effective immune responses and tend to have poorer survival. A new phase in cancer-targeted therapy will be particularly difficult, but especially needed, for AML patients whose tumors lack cytogenetic abnormalities and detectable immunogenic LAA expression and whose survival rates are notably reduced
SSX2IP, RHAMM, survival, acute myeloid leukaemia, survivin
1203-1204
Guinn, B.
67391e0b-159a-4a5e-b027-da20ccaee04e
Greiner, J.
d9bc880b-1515-4291-b794-dd81b4e28c86
Schmitt, M.
88acb369-7a36-46cb-b442-fb4f952f5fee
Mills, K.I.
2e4e2765-fc9e-4fd6-a9c7-fe6d865fe732
15 January 2009
Guinn, B.
67391e0b-159a-4a5e-b027-da20ccaee04e
Greiner, J.
d9bc880b-1515-4291-b794-dd81b4e28c86
Schmitt, M.
88acb369-7a36-46cb-b442-fb4f952f5fee
Mills, K.I.
2e4e2765-fc9e-4fd6-a9c7-fe6d865fe732
Guinn, B., Greiner, J., Schmitt, M. and Mills, K.I.
(2009)
Elevated expression of the leukaemia associated antigen SSX2IP predicts good survival in acute myeloid leukaemia patients who lack detectable cytogenetic rearrangements.
Blood, 113 (5), .
(doi:10.1182/blood-2008-09-178848).
Abstract
Greiner et al have previously described a positive association between elevated leukemia-associated antigen (LAA) expression (RHAMM, G250/CA9, and PRAME) and survival in 116 acute myeloid leukemia (AML) patients by microarray. We have analyzed 312 presentation AML samples using 199 133A chips and 113 Plus2 chips and segregated AML patients based on above- and below-median levels of expression of the LAA synovial sarcoma X breakpoint 2–interacting protein (SSX2IP). Analysis of Kaplan-Meier curves showed an association between elevated SSX2IP expression and improved survival times (log-rank test, P = .05). We found that SSX2IP expression did not predict the survival of AML patients who had detectable cytogenetic abnormalities; however, it was significantly associated with improved survival rates in patients with no detectable cytogenetic rearrangements (log-rank test, n = 180; P = .007). We also found a correlation between elevated SSX2IP expression and other clinical parameters that are considered to be good prognostic markers: days in remission (log-rank test, P = .03), age at diagnosis (< 60 years; t test, P = .003), and FLT3 WT (t test, P = .004). When we examined SSX2IP together with the expression of other LAAs known to be associated with improved survival, we found a significant correlation with SURVIVIN (Pearson correlation, P = 3.97 x 10–5) and RHAMM (Pearson correlation, P = 4.3 x 10–5). Other groups suggested that the expression of distinct LAAs on leukemic blasts may lead to the eradication of residual disease after intensive chemotherapy. RHAMM and Survivin, like SSX2IP, have increased expression in proliferating cells while RHAMM and SSX2IP are both expressed on the surface of malignant cells. There appears to be a small but growing group of LAAs that are coexpressed in AML patients and are associated with improved survival. We examined whether having 1 or more of SSX2IP, Survivin, or RHAMM affected survival in patients with a normal karyotype and found that having expression of none, 1, 2 or all 3 of these LAAs was a significant prognostic indicator (log-rank test, P = .021, respectively). With regard to the presence of cytogenetic abnormalities, these appear to supersede the influence of elevated LAA expression on prognosis.
In summary, we have found that SSX2IP expression at disease presentation predicts good survival in AML patients with no detectable cytogenetic rearrangements. This may, in part, explain why patients with low LAA expression (often the elderly) fail to elicit effective immune responses and tend to have poorer survival. A new phase in cancer-targeted therapy will be particularly difficult, but especially needed, for AML patients whose tumors lack cytogenetic abnormalities and detectable immunogenic LAA expression and whose survival rates are notably reduced
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Published date: 15 January 2009
Keywords:
SSX2IP, RHAMM, survival, acute myeloid leukaemia, survivin
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Local EPrints ID: 71029
URI: http://eprints.soton.ac.uk/id/eprint/71029
ISSN: 0006-4971
PURE UUID: ed6b7c67-fe45-45c4-8493-71a9af17bee9
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Date deposited: 14 Dec 2009
Last modified: 13 Mar 2024 20:17
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Author:
B. Guinn
Author:
J. Greiner
Author:
M. Schmitt
Author:
K.I. Mills
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