Loss of p53 Is a Marker of Progression in Plasma Cell Neoplasias and Is a Negative Prognostic Factor in Relapsed Disease.

Molnar, Soledad; Zepeda, Victor J Jimenez; Wier, Scott Van; Braggio, Esteban; Kuehl, Michael; Price-Troska, Tammy; Ahmann, Greg; Rempel, Rachel E.; Henderson, Kim; Rajkumar, S. Vincent; Greipp, Philip R.; Auclair, Daniel; Carpten, John D.; Baker, Angela; Stewart, Keith; Bergsagel, P. Leif; Chng, Wee Joo; Fonseca, Rafaël

doi:10.1182/blood.v112.11.1663.1663

Cited by 2 publications

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“…The number of prior lines of therapy was previously reported as 1 of the major factors to predict survival [12]. This is likely a surrogate marker for the presence of chemoresistant disease or the persistence of subclinical cumulative toxicity from prior therapies but also could reflect an increase of acquired genetic aberrations such as p53 deletion [25].…”

Section: Discussionmentioning

confidence: 97%

Second Autologous Stem Cell Transplantation as Salvage Therapy for Multiple Myeloma: Impact on Progression-Free and Overall Survival

Jiménez-Zepeda

Mıkhael

Winter

et al. 2012

Biology of Blood and Marrow Transplantation

108

101

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The role of a second autologous stem cell transplant (ASCT) as salvage therapy is unclear, particularly with the availability of novel agents to treat progressive multiple myeloma (MM). We retrospectively reviewed all MM patients who received a second ASCT as salvage therapy at our center from March 1992 to December 2009. Eighty-one MM patients received a second ASCT for relapsed MM. The median time to relapse after first transplant was 39 months (9.83-100). All patients received reinduction therapy before the second ASCT. The high-dose regimen given before the second ASCT consisted of melphalan (MEL) alone in the majority. Complete response, very good partial response, and partial response were seen in 7.7%, 39.7%, and 50%, respectively, at day 100 post-ASCT; the median time to relapse after the second ASCT was 19 months. Early deaths occurred in 2.6%. Median progression-free survival (PFS) based on the time to myeloma relapse after first ASCT was 9.83 months (relapse ≤ 24 months) and 17.3 months (relapse ≥ 24 months) (P < .05). Median overall survival (OS) was 28.47 months (relapse ≤ 24 months) and 71.3 months (relapse >24 months) (P = .006). Second ASCT is a feasible and safe option for salvage therapy in MM. The best outcome was observed in patients whose time to progression was >24 months after first ASCT, as these patients had a subsequent PFS lasting over 1 year and an OS of almost 6 years.

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Section: Discussionmentioning

confidence: 97%

Second Autologous Stem Cell Transplantation as Salvage Therapy for Multiple Myeloma: Impact on Progression-Free and Overall Survival

Jiménez-Zepeda

Mıkhael

Winter

et al. 2012

Biology of Blood and Marrow Transplantation

108

101

View full text Add to dashboard Cite

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“…On the other hand, it is unclear why plasma cells escape from the bone marrow and become PCL. Emergence of TP53 deletion/mutations denotes progression genetic events in MM (22). The prevalence of TP53 deletion detected either by FISH or by array CGH is approximately 80% in PCL, and this genetic abnormality is thought to be responsible for the presence of extramedullary disease in MM.…”

Section: Discussionmentioning

confidence: 99%

Chromosome abnormalities defined by conventional cytogenetics in plasma cell leukemia: what have we learned about its biology?

Jiménez-Zepeda

Neme-Yunes

Braggio

2011

European Journal of Haematology

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Cancer cells are characterized by having chromosomal abnormalities. The number of aberrations and the specific chromosomes affected are likely correlated with tumor progression. In this study, we analyzed the karyotype of 126 plasma cell leukemia (PCL) patients to identify the most frequently occurring imbalances and to design a model of karyotypic evolution. The Mitelman database of chromosome was searched and abnormal karyotypes were assessed. The main clones were analyzed and chromosomal gains and losses were used to design a model of genetic acquisition based on the calculation of a variable called time to occurrence. Our comprehensive study of genetic abnormalities of a large number of PCL karyotypes suggests that PCL is mainly characterized by the presence of whole chromosome losses as well as IgH rearrangements which is similar to that observed in non-hyperdiploid multiple myeloma (MM). Temporal analysis suggests that most PCL have around 10 abnormalities at diagnosis. It is possible that accumulation of abnormalities such as 17p13 (TP53) and 1p losses may trigger the extramedullary features of PCL. Our study demonstrates that cytogenetics is a valuable tool to evaluate the role of genetic imbalances on karyotypic evolution by using a mathematical model.

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Loss of p53 Is a Marker of Progression in Plasma Cell Neoplasias and Is a Negative Prognostic Factor in Relapsed Disease.

Cited by 2 publications

References 0 publications

Second Autologous Stem Cell Transplantation as Salvage Therapy for Multiple Myeloma: Impact on Progression-Free and Overall Survival

Second Autologous Stem Cell Transplantation as Salvage Therapy for Multiple Myeloma: Impact on Progression-Free and Overall Survival

Chromosome abnormalities defined by conventional cytogenetics in plasma cell leukemia: what have we learned about its biology?

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