Gene rearrangement study for minimal residual disease
               monitoring in children with acute lymphocytic leukemia

Assumpção, Juliana Godoy; Paula, Francisco Danilo Ferreira; Xavier, Sandra Guerra; Murao, Mitiko; Aguirre Neto, Joaquim Caetano de; Dutra, Álvaro Pimenta; Lima, Eduardo Ribeiro; Oliveira, Benigna Maria de; Viana, Marcos Borato

doi:10.5581/1516-8484.20130115

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Revista Brasileira de Hematologia e Hemoterapia

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Sumário

ORIGINAL ARTICLES • Rev Bras Hematol Hemoter 35 (5) • 2013 • https://doi.org/10.5581/1516-8484.20130115 copy

Gene rearrangement study for minimal residual disease monitoring in children with acute lymphocytic leukemia

Authorship SCIMAGO INSTITUTIONS RANKINGS

OBJECTIVE

To detect markers for minimal residual disease monitoring based on conventional polymerase chain reaction for immunoglobulin, T-cell receptor rearrangements and the Sil-Tal1 deletion in patients with acute lymphocytic leukemia.

METHODS

Fifty-nine children with acute lymphocytic leukemia from three institutions in Minas Gerais, Brazil, were prospectively studied. Clonal rearrangements were detected by polymerase chain reaction followed by homo/heteroduplex clonality analysis in DNA samples from diagnostic bone marrow. Follow-up samples were collected on Days 14 and 28-35 of the induction phase. The Kaplan-Meier and multivariate Cox methods were used for survival analysis.

RESULTS

Immunoglobulin/T-cell receptor rearrangements were not detected in 5/55 children screened (9.0%). For precursor-B acute lymphocytic leukemia, the most frequent rearrangement was IgH (72.7%), then TCRG (61.4%), and TCRD and IgK (47.7%); for T-acute lymphocytic leukemia, TCRG (80.0%), and TCRD and Sil-Tal deletion (20.0%) were the most common. Minimal residual disease was detected in 35% of the cases on Day 14 and in 22.5% on Day 28-35. Minimal residual disease on Day 28-35, T-acute lymphocytic leukemia, and leukocyte count above 50 x 10⁹/L at diagnosis were bad prognostic factors for leukemia-free survival in univariate analysis. Relapse risk for minimal residual disease positive relative to minimal residual disease negative children was 8.5 times higher (95% confidence interval: 1.02-70.7).

CONCLUSION

Immunoglobulin/T-cell receptor rearrangement frequencies were similar to those reported before. Minimal residual disease is an independent prognostic factor for leukemia-free survival, even when based on a non-quantitative technique, but longer follow-ups are needed.

Precursor cell lymphoblastic leukemia-lymphoma; Neoplasm, residual; Gene rearrangement; Polymerase chain reaction

Variable		%
Age (n = 59)
	1-9 years	62.7
	≥ 9 years	37.3
White blood cell count at diagnosis (n = 59)
	< 50x109/L	83.1
	≥ 50x109/L	16.9
Central nervous system status at diagnosis (n = 47)
	CNS 3	0
	CNS1 or 2	100
White blood cell count on Day 7 (n = 46)
	< 5x10⁹/L	80.4
	≥ 5x10⁹/L	19.6
Bone marrow on Day 14 (n = 33)
	M1/M2	78.8
	M3	21.2
Bone marrow on Day 28-35 (n = 57)
	M1	96.5
	M2/M3	3.5
Response (n = 48)
	Good responder	72.9
	Poor responder⁽¹ 1 Poor responder: patients who fulfilled one or more of the following criteria during the phase of remission induction: white blood cell count on Day 7 ≥ 5x109/L, bone marrow M3 (> 25% blasts) on D14 or bone marrow M2 or M3 (> 5% and 25% blasts, respectively) on D28/D35. ⁾	27.1
Final risk group (n = 59)
	Low risk	35.6
	High risk	64.4
Immunophenotype (n = 59)
	Precursor B-lineage	81.4
	T-lineage	18.6
BCR-ABL fusion transcript (n = 51)
	Positive	5.9
	Negative	94.1
Event at induction (n = 59)
	Complete remission	96.6
	Death during induction	3.4

Gene Rearrangement		Frequency
IgH
	FR3A - LJH	32/44 (72.7%)
IgK
	VkI - intron, Kde	7/42 (16.3%)
	VkII, VkIII - Kde	16/44 (36.4%)
TCRG
	Vγ2, Vγ8 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	17/44 (38.6%)
	Vγ3, Vγ5- Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	9/44 (20.5%)
	Vγ9 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	11/44 (25%)
TCRD
	Vd2 - Dd3	20/44 (45.5%)
	Dd2 - Dd3	4/43 (9.3%)

Gene Rearrangement		Frequency
TCRG
	Vγ2, Vγ8 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	6/11 (54.6%)
	Vγ3, Vγ5- Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	2/11 (18.2%)
	Vγ9 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	0/10 (0%)
	Vγ10 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	1/10 (10%)
	Vγ11 - Jγ1.3/2.3, Jγ1.1/2.1, Jγ1.2	1/10 (10%)
TCRD
	Vd2 - Dd3	0/11 (0%)
	Vd2 - Jd1	0/10 (0%)
Vd3 - Jd1
	Sil-Tal	2/10 (20%)
	Sil-Tal1	2/10 (20%)

Variable		Percentage
MRD Day 14 (n = 29)
	Negative	19 (65.5%)
	Positive	10 (34.5%)
MRD Day 28-35 (n = 40)
	Negative	31 (77.5%)
	Positive	9 (22.5%)
MRD Day 14 and Day 28-35 (n = 24)
	Negative Day 14 and Day 28	15 (60%)
	Positive Day 14 and negative Day 28	5 (20%)
	Positive Day 14 and Day 28	4 (16%)

Variable	B coefficient	Standard error	p-value	Relative risk¹ 1 Relative risk refers to leukemia relapse in T-acute lymphocytic leukemia relative to precursor-B acute lymphocytic leukemia
Variable	B coefficient	Standard error	p-value	Estimated	95% CI
Immunophenotype	1.577	1.07	0.14	4.84	0.59-39.58
WBC² 2 White blood cells (WBC) > 50 x 109/L relative to WBC < 50 x 109/L at diagnosis	1.588	0.99	0.11	4.89	0.70-34.03
MRD³ 3 Positive minimal residual disease (MRD) relative to negative MRD on Day 28-35	2.141	1.08	0.048	8.51	1.02-70.69

Associação Brasileira de Hematologia e Hemoterapia e Terapia Celular R. Dr. Diogo de Faria, 775 cj 114, 04037-002 São Paulo/SP/Brasil, Tel. (55 11) 2369-7767/2338-6764 - São Paulo - SP - Brazil
E-mail: secretaria@rbhh.org

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[1] Corresponding author: Juliana Godoy Assumpção. Universidade Federal de Minas Gerais - UFMG. Laboratório de Hematologia Molecular. Av. Alfredo Balena 190, sala 149. 30130-100 Belo Horizonte, MG, Brazil. Phone: 55 31 34099229. julianaassumpcao@yahoo.com.br