Shortened survival after relapse in T-cell acute lymphoblastic leukemia patients with p16/p15 deletions

Mitchell B. Diccianni; Ayse Batova; John Yu; Thai Vu; Jeanette Pullen; Michael Amylon; Brad H. Pollock; Alice L. Yu

doi:10.1016/S0145-2126(97)00007-6

Shortened survival after relapse in T-cell acute lymphoblastic leukemia patients with p16/p15 deletions

Mitchell B. Diccianni, Ayse Batova, John Yu, Thai Vu, Jeanette Pullen, Michael Amylon, Brad H. Pollock, Alice L. Yu

Research output: Contribution to journal › Article › peer-review

35 Scopus citations

Abstract

p16 Alterations were detected in > 60% of 103 primary T-ALL samples. In paired diagnosis-relapse patient samples, 80% of the relapse samples with p16 deletion were deleted at diagnosis. When p16 was homozygously deleted, p15 gene alterations were found in 72% of the diagnosis T-ALL patient samples, increasing significantly to 100% at relapse. Alterations of p18 were not detected. No clinical significance of p15/p16 gene deletion in diagnosis T-ALL was found with respect to white blood cell (WBC) count, incidence of mediastinal mass, rate of relapse, duration of first remission or event-free survival. In relapse T-ALL, however, patients with p16 deletion experienced a significantly shorter duration of post-relapse survival, demonstrating that p16 deletion is clinically significant in T-ALL.

Original language	English (US)
Pages (from-to)	549-558
Number of pages	10
Journal	Leukemia Research
Volume	21
Issue number	6
DOIs	https://doi.org/10.1016/S0145-2126(97)00007-6
State	Published - Jun 1997
Externally published	Yes

Keywords

p15
p16
p18
Prognosis
Relapse
T-ALL

ASJC Scopus subject areas

Hematology
Oncology
Cancer Research

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10.1016/S0145-2126(97)00007-6

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title = "Shortened survival after relapse in T-cell acute lymphoblastic leukemia patients with p16/p15 deletions",

abstract = "p16 Alterations were detected in > 60% of 103 primary T-ALL samples. In paired diagnosis-relapse patient samples, 80% of the relapse samples with p16 deletion were deleted at diagnosis. When p16 was homozygously deleted, p15 gene alterations were found in 72% of the diagnosis T-ALL patient samples, increasing significantly to 100% at relapse. Alterations of p18 were not detected. No clinical significance of p15/p16 gene deletion in diagnosis T-ALL was found with respect to white blood cell (WBC) count, incidence of mediastinal mass, rate of relapse, duration of first remission or event-free survival. In relapse T-ALL, however, patients with p16 deletion experienced a significantly shorter duration of post-relapse survival, demonstrating that p16 deletion is clinically significant in T-ALL.",

keywords = "p15, p16, p18, Prognosis, Relapse, T-ALL",

author = "Diccianni, {Mitchell B.} and Ayse Batova and John Yu and Thai Vu and Jeanette Pullen and Michael Amylon and Pollock, {Brad H.} and Yu, {Alice L.}",

note = "Funding Information: acknowledge the PGG Cell Bank at St. Jude Children{\textquoteright}s Hospital for providing some cryopreserved T-ALL samples at diagnosis. This work is supported by Grants UlOCA28439 and FDA001129 (ALY)andDK40218 (JY),andinpartbyagrant from the General Clinical Research Center program, MO1 RRO0827. MBD is supported by a NIH postdoctoral training Grant No. T32 CA 09290. AB is supported by NIH Grant for training and research on blood and blood disease No. 2T32-HLo7107.",

year = "1997",

month = jun,

doi = "10.1016/S0145-2126(97)00007-6",

language = "English (US)",

volume = "21",

pages = "549--558",

journal = "Leukemia Research",

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T1 - Shortened survival after relapse in T-cell acute lymphoblastic leukemia patients with p16/p15 deletions

AU - Diccianni, Mitchell B.

AU - Batova, Ayse

AU - Yu, John

AU - Vu, Thai

AU - Pullen, Jeanette

AU - Amylon, Michael

AU - Pollock, Brad H.

AU - Yu, Alice L.

N1 - Funding Information: acknowledge the PGG Cell Bank at St. Jude Children’s Hospital for providing some cryopreserved T-ALL samples at diagnosis. This work is supported by Grants UlOCA28439 and FDA001129 (ALY)andDK40218 (JY),andinpartbyagrant from the General Clinical Research Center program, MO1 RRO0827. MBD is supported by a NIH postdoctoral training Grant No. T32 CA 09290. AB is supported by NIH Grant for training and research on blood and blood disease No. 2T32-HLo7107.

PY - 1997/6

Y1 - 1997/6

N2 - p16 Alterations were detected in > 60% of 103 primary T-ALL samples. In paired diagnosis-relapse patient samples, 80% of the relapse samples with p16 deletion were deleted at diagnosis. When p16 was homozygously deleted, p15 gene alterations were found in 72% of the diagnosis T-ALL patient samples, increasing significantly to 100% at relapse. Alterations of p18 were not detected. No clinical significance of p15/p16 gene deletion in diagnosis T-ALL was found with respect to white blood cell (WBC) count, incidence of mediastinal mass, rate of relapse, duration of first remission or event-free survival. In relapse T-ALL, however, patients with p16 deletion experienced a significantly shorter duration of post-relapse survival, demonstrating that p16 deletion is clinically significant in T-ALL.

AB - p16 Alterations were detected in > 60% of 103 primary T-ALL samples. In paired diagnosis-relapse patient samples, 80% of the relapse samples with p16 deletion were deleted at diagnosis. When p16 was homozygously deleted, p15 gene alterations were found in 72% of the diagnosis T-ALL patient samples, increasing significantly to 100% at relapse. Alterations of p18 were not detected. No clinical significance of p15/p16 gene deletion in diagnosis T-ALL was found with respect to white blood cell (WBC) count, incidence of mediastinal mass, rate of relapse, duration of first remission or event-free survival. In relapse T-ALL, however, patients with p16 deletion experienced a significantly shorter duration of post-relapse survival, demonstrating that p16 deletion is clinically significant in T-ALL.

KW - p15

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KW - Prognosis

KW - Relapse

KW - T-ALL

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Shortened survival after relapse in T-cell acute lymphoblastic leukemia patients with p16/p15 deletions

Abstract

Keywords

ASJC Scopus subject areas

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