Precursor B-lineage acute lymphoblastic leukemia patients with aberrant natural killer cell and T cell - lineage antigen expression: experience from a tertiary cancer care center

Bommannan, Karthik; Arumugam, Jhansi Rani; Radhakrishnan, Venkatraman; Kalaiyarasi, Jayachandran Perumal; Mehra, Nikita; Sagar, Tenali Gnana; Sundersingh, Shirley

doi:10.1016/j.htct.2020.08.012

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Hematology, Transfusion and Cell Therapy

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Original article • Hematol., Transfus. Cell Ther. 44 (2) • 2022 • https://doi.org/10.1016/j.htct.2020.08.012 copy

Precursor B-lineage acute lymphoblastic leukemia patients with aberrant natural killer cell and T cell - lineage antigen expression: experience from a tertiary cancer care center

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Introduction

Flow cytometric immunophenotyping (FCI) plays a major role in diagnosing hematologic malignancies. In patients diagnosed with precursor B-lineage acute lymphoblastic leukemia (B-ALL), expression of certain non-lineage/cross lineage antigens is of prognostic and cytogenetic relevance. There is a paucity of studies that have comprehensively analyzed the clinical and laboratory profiles of B-ALL patients showing aberrant T/natural killer (NK) cell antigen expression.

Materials and methods

This is a prospective study where 152 consecutive B-ALL patients were analyzed for aberrant expression of T/NK cell antigens (CD1a, CD5, CD4, CD7, CD8 and CD56) by FCI. The clinical and laboratory profile of these T/NK-cell antigen-expressing B-ALL patients was statistically analyzed against conventional B-ALL patients.

Results

In our B-ALL cohort, CD5, CD7 and CD56 expression were observed in one, six and nine patients, respectively. CD56-expressing B-ALL patients were predominantly children (89%) and presented as standard clinical risk (p = 0.010) disease with frequent ETV6-RUNX1 fusion (p = 0.021) positivity. On the contrary, CD7-expressing B-ALL patients were adolescent-young adult/adult-age skewed (83%) and had an adverse cytogenetic profile (p = 0.001), especially for the frequent presence of BCR-ABL1 fusion (p = 0.004) and KMT2A rearrangement (p = 0.045). CD7-expressing B-ALL patients had inferior event-free survival (p = 0.040) than their CD56-expressing counterparts, but there was no significant difference in the overall survival (p = 0.317).

Conclusion

In comparison to conventional B-ALL patients, there are significant differences in the age, cytogenetic profile and event-free survival of T/NK-cell antigen-expressing B-ALL patients.

Keywords
CD56 positive precursor B lineage acute lymphoblastic leukemia; CD7 positive precursor B lineage acute lymphoblastic leukemia; Precursor B lineage acute lymphoblastic leukemia

B-ALL patient category		All patients (n = 152)	CD56 expression		CD7 expression		P-value
			CD56- (n = 143)	CD56+ (n = 9)	CD7- (n = 146)	CD7+ (n = 6)	CD56+ vs CD56-	CD7+ vs CD7-	CD56+ vs CD7+
Median age (range) in years		10 (0.2-64)	10 (0.2-64)	7 (2-62)	10 (0.2-64)	20 (3-50)	0.336	0.086	0.088
Age Group	Pediatric	94	86	8	93	1	0.188	0.021	0.014
	AYA	32	32	0	29	3
	Adult	26	25	1	24	2
Sex (Male: Female)		1.8:1	1.6:1	2:1	1.7:1	2:1	0.822	0.856	1.00
Pro B-ALL (%)		8 (5)	7 (5)	1 (11)	7 (5)	1 (17)	0.394	0.202	0.756
Median (range) Hb in g/L		73 (22-149)	73(25-149)	67 (22-90)	73 (22-149)	71 (5-10)	0.336	0.921	0.388
Median(range) WBC count X10⁹/L		10.3 (0.3-587)	10.3 (0.3−586)	6.8 (3.3−26.4)	10.2 (.3-587)	21.2 (3.5-175)	0.571	0.241	0.181
Median (range) Platelet X10⁹/L		50 (10-563)	50 (10−563)	50 (20−457)	50 (10−563)	38 (15−71)	0.726	0.244	0.224
Median (range) BM blast %		89 (55−99)	89(78−94)	85(66−97)	89 (55−99)	82 (66−98)	0.926	0.869	0.864
Median (range) PB blast %		49 (4−98)	50(11−84)	41(4−88)	48 (6−98)	86 (5−98)	0.732	0.144	0.142
Splenomegaly (%)		67/152 (44)	63/143 (44)	4/9 (44)	66/146 (45)	2/6 (33)	0.501	0.567	0.398
Hepatomegaly (%)		56/152 (37)	52/143 (36)	4/9 (44)	55/146 (38)	1/6 (17)	0.626	0.296	0.246
Lymphadenopathy (%)		45/152 (30)	41/143 (28)	4/9 (44)	43/146 (30)	2/6 (33)	0.315	0.838	0.667
CNS involvement at diagnosis (%)		5/138 (4)	5/129 (4)	0/9 (0)	5/131 (4)	0/0 (0)	0.569	0.626	NA
Ploidy (%)	Diploid	84/124 (68)	75/115 (65)	9/9 (100)	78/118 (66)	6/6 (100)	0.728	0.864	NA
	High Hyperdiploid	18/124 (14)	18/115 (16)	0/9 (0)	18/118 (15)	0/6 (0)
	Low Hyperdiploid	14/124 (11)	14/115 (12)	0/9 (0)	14/118 (12)	0/6 (0)
	High Hypodiploid	04/124 (3)	4/115 (3.5)	0/9 (0)	4/118 (3)	0/6 (0)
	Low Hypodiploid	01/124 (1)	1/115 (1)	0/9 (0)	1/118 (1)	0/6 (0)
	Near Triploid	01/124 (1)	1/115 (1)	0/9 (0)	1/118 (1)	0/6 (0)
	Near Tetraploid	02/124 (2)	2/115 (2)	0/9 (0)	2/118 (2)	0/6 (0)
NCI High-risk disease (%)		95/152 (62.5)	93/143 (65)	2/9 (22)	90/146 (62)	5/6 (83)	0.010	0.282	0.020
BCR-ABL1 fusion positive (%)		16/133 (12)	16/124 (13)	0/9(0)	13/127 (10)	3/6 (40)	0.278	0.004	0.024
ETV6-RUNX1 fusion positive (%)		14/133 (10.5)	11/124 (9)	3/9 (33)	13/127 (10)	1/6 (17)	0.021	0.616	0.475
KMT2A rearranged (%)		04/133 (3)	04/124 (3)	0/9 (0)	03/127 (2)	1/6 (17)	0.584	0.045	0.205
TCF3-PBX1 fusion positive (%)		05/133 (4)	05/124 (4)	0/9 (0)	05/127 (4)	0/6 (0)	0.539	0.620	NA
High Risk cytogenetics (%)		21/133 (16)	21/124 (17)	0/9 (0)	17/127 (13)	4/6 (67)	.202	0.001	0.006
End induction MRD positive (%)		56/135 (41)	53/127 (42)	3/8 (37.5)	52/129 (40)	4/6 (67)	0.814	0.200	0.280
Induction failure (%)		05/135 (4)	5/127 (4)	0/8 (0)	4/129 (3)	1/6 (17)	0.568	0.061	0.205
Relapse (%)		13/135 (10)	13/127 (10)	0/8 (0)	12/129 (9)	1/6 (17)	0.344	0.468	0.205
Adverse events (%)		25/138 (18)	25/130 (19)	0/8 (0)	22/129 (17)	3/6 (50)	0.170	0.024	0.018

Literature		Current	Hussein et al.³3 Hussein S, Gill KZ, Sireci AN, Colovai AI, Small T, Emmons FN, et al. Aberrant T-cell antigen expression in B lymphoblastic leukaemia. Br J Haematol. 2011;155(4):449-56.	Seegmiller et al.²2 Seegmiller AC, Kroft SH, Karandikar NJ, McKenna RW. Characterization of immunophenotypic aberrancies in 200 cases of B acute lymphoblastic leukemia. Am J Clin Pathol. 2009;132(6):940-9.	Aref et al.⁴4 Aref S, Azmy E, El-Bakry K, Ibrahim L, Mabed M. Prognostic impact of CD200 and CD56 expression in adult acute lymphoblastic leukemia patients. Hematology. 2018;23(5):263-70.
Age group evaluated		All	All	All	AYA and Adult
Year		2019	2011	2009	2017
Country		India	USA	USA	Egypt
B-ALL patients evaluated		152	134	197	70
CD56+ patients (%)		9 (6)	3 (2.2)	10 (5)	7 (10)
Median age (Range) in years		7(2−62)	16 (13−16)	NA	NA (28−50)
Age Group (n)	Ped	8	01	09	00
	AYA	0	02	00	07^c c Distinction between AYA and Adults not available.
	Adult	1	00	01	07^c c Distinction between AYA and Adults not available.
Sex (Male: Female)		2:1	2:1	NA	1.3:1
Median (range) Hb in g/L		67(22−90)	NA	NA	77 (68−106)
Median(range) WBC count X10⁹/L		6.8 (3.3−26.4)	NA	NA	18.3 (1.7−113)
Median (range) Platelet X10⁹/L		50 (20−457)	NA	NA	140 (26−397)
Median (range) BM blast %		85(66−97)	NA	NA	80 (55−93)
Median (range) PB blast %		41(4−88)	NA	NA	90 (80−90)
Splenomegaly (%)		4/9 (44)	NA	NA	2/7 (29)
Hepatomegaly (%)		4/9 (44)	NA	NA	2/7 (29)
Lymphadenopathy (%)		4/9 (44)	NA	NA	4/7 (57)
CNS disease at baseline (%)		0/9 (0)	NA	NA	6/7 (87)
Diploidy (%)		9/9 (100)	NA	NA	NA
High-Risk cytogenetics (%)		0/9 (0)	1^a a TP53 deleted. /3 (33)	NA	4/7 (57)
BCR-ABL1 fusion-positive (%)		0/9(0)	0/3	NA	4/7 (57)
ETV6-RUNX1 fusion-positive (%)		3/9 (33)	0/3	(27)	NA
KMT2A rearranged (%)		0/9 (0)	0/3	NA	NA
TCF3-PBX1 fusion-positive (%)		0/9 (0)	0/3	NA	NA
End induction MRD-positive (%)		3/8 (37.5)	NA	NA	NA
Induction failure (%)		0/8 (0)	1/3 (33)	NA	2/7 (29)
Induction death (%)		0/8 (0)	0/3 (0)	NA	3/7 (43)
Relapse (%)		0/8 (0)	0/1^b b Data of one patient as One patient left against medical advice and another had induction failure and was also treatment-refractory. (0)	NA	NA

Literature		Current	Hussein et al.³3 Hussein S, Gill KZ, Sireci AN, Colovai AI, Small T, Emmons FN, et al. Aberrant T-cell antigen expression in B lymphoblastic leukaemia. Br J Haematol. 2011;155(4):449-56.	Seegmiller et al.²2 Seegmiller AC, Kroft SH, Karandikar NJ, McKenna RW. Characterization of immunophenotypic aberrancies in 200 cases of B acute lymphoblastic leukemia. Am J Clin Pathol. 2009;132(6):940-9.
Age group evaluated		All	All	All
Year		2019	2011	2009
Country		India	USA	USA
B-ALL patients evaluated		152	134	197
CD7+ patients (%)		6 (4)	6 (4.4)	4 (2)
Median age (Range) in years		20 (3−50)	5.4 (0.4-25)	NA
Age Group (n)	Ped	1	05	01
	AYA	3	01
	Adult	2	00	03
Sex (Male: Female)		2:1	1:2	NA
Median (range) Hb in g/L		71 (5-10)	NA	NA
Median(range) WBC count X10⁹/L		21.2 (3.5-175)	NA	NA
Median (range) Platelet X10⁹/L		38 (15-71)	NA	NA
Median (range) BM blast %		82 (66-98)	NA	NA
Median (range) PB blast %		86 (5-98)	NA	NA
Splenomegaly (%)		2/6 (33)	NA	NA
Hepatomegaly (%)		1/6 (17)	NA	NA
Lymphadenopathy (%)		2/6 (33)	NA	NA
CNS disease at diagnosis		0/0 (0)	NA	NA
Diploidy (%)		6/6 (100)	NA
High-Risk cytogenetics (%)		4/6 (67)	4/6^a a One patient had CDKND2A deletion. (67)	NA
BCR-ABL1 fusion-positive (%)		3/6 (40)	0/6 (0%)	NA
ETV6-RUNX1 fusion-positive (%)		1/6 (17)	0/6 (0%)	NA
KMT2A rearranged (%)		1/6 (17)	3/6 (50%)	NA
TCF3-PBX1 fusion-positive (%)		0/6 (0)	0/6 (0%)	NA
End induction MRD-positive (%)		4/6 (67)	NA	NA
Induction failure (%)		1/6 (17)	0/6	NA
Induction death (%)		0/6 (0)	0/6 (0)	NA
Relapse (%)		1/6 (17)	4/6 (67)	NA

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[1] *Corresponding author at: Department of Oncopathology, Cancer Institute (W.I.A,) Adyar, Chennai, 600020 India. E-mail address: bkkb87@gmail.com (K. Bommannan).