<i>TP</i>53 and <i>p</i>21 (CDKN1A) polymorphisms and the risk of systemic lupus erythematosus

Macedo, Jacyara Maria Brito; Silva, Amanda Lima; Pinto, Amanda Chaves; Landeira, Leandro Ferreira Lopes; Portari, Elyzabeth Avvad; Santos-Rebouças, Cintia Barros; Klumb, Evandro Mendes

doi:10.1186/s42358-023-00320-4

Jacyara Maria Brito Macedo

conceived the study design

acquired financial support for the project

supervised the laboratory work and the statistical analysis

discussed the results

participated in the manuscript preparation and revision

Department of Biochemistry, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0002-4976-9318

Amanda Lima Silva

the analysis of p21 polymorphism

performed the statistical analysis

participated in the discussion of results and manuscript preparation

Department of Biochemistry, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0002-2143-4719

Amanda Chaves Pinto

DNA extraction from peripheral blood samples and DNA sequencing and participated in the manuscript preparation

Department of Biochemistry, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0002-4372-096X

Leandro Ferreira Lopes Landeira

the analysis of TP53 polymorphisms

Department of Biochemistry, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0001-5121-8139

Elyzabeth Avvad Portari

the analysis of TP53 and p21 polymorphisms

Department of Pathological Anatomy, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

Department of Pathology, Fernandes Figueira Institute - FIOCRUZ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0003-2372-0898

Cintia Barros Santos-Rebouças

the study design, carried out the analysis of TP53 and p21 polymorphisms and participated in the manuscript preparation and revision

Department of Pathological Anatomy, State University of Rio de Janeiro - UERJ, Rio de Janeiro, Brazil.

http://orcid.org/0000-0003-4729-2373

Evandro Mendes Klumb ^**Correspondence: Evandro Mendes Klumb klumb@uol.com.br

financial support for the project

participated in the clinical patient selection and clinical data analysis and participated in the manuscript preparation and revision

Department of Rheumatology, Pedro Ernesto University Hospital, State University of Rio de Janeiro - UERJ, Boulevard 28 de Setembro, 87, Vila Isabel, Rio de Janeiro, RJ CEP 20551-030, Brazil.

http://orcid.org/0000-0001-9546-3144

*Correspondence: Evandro Mendes Klumb klumb@uol.com.br

Competing interests

The authors declare that they have no competing interests.

Figures (1)
Tables (5)

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Fig. 1 Molecular analysis of polymorphisms in the TP53 and p21 (CDKN1A) genes. Left: A TP53 rs1042522 (G > C). Photography of an ethidium bromide-stained agarose gel (2%) showing PCR-fistUI RFLP patterns. Lane 1: 50 bp ladder (INVITROGEN); lanes 2, 3 and 4: genotypes rs1042522 CC (one fragment of 492 or 476 bp), rs1042522 GC (three fragments of 492 or 476, 305 or 284 and 187 bp) and rs1042522 GG (two fragments of 305 or 284 bp and 187 bp), respectively. B TP53 rs17878362 (16 bp Del/Ins). Photography of an ethidium bromide-stained polyacrylamide gel (8%) showing PCR patterns. Lane 1: 50 bp ladder (INVITROGEN); lanes 2, 3 and 4: genotypes rs17878362 A1A1 (one fragment of 492 bp), rs17878362 A1A2 (two fragments of 492 and 476 bp) and rs17878362 A2A2 (one fragment of 476 bp), respectively. C p21 rs1801270 (C > A). Photography of an ethidium bromide-stained polyacrylamide gel (8%) showing PCR-A/w26I RFLP patterns. Lane 1: 50 bp ladder (INVITROGEN); lanes 2, 3 and 4: genotypes rs1801270 CC (two fragments of 105 and 74 bp), rs1801270 CA (three fragments of 179, 105 and 74 bp) and rs1801270 AA (one fragment of 179 bp), respectively. D p21 rs1059234 (C >T) polymorphism. Photography of an ethidium bromide-stained polyacrylamide gel (8%) showing PCR-PstI RFLP patterns. Lane 1: 50 bp ladder (INVITROGEN); lanes 2, 3 and 4: genotypes rs1059234 CC (two fragments of 115 and 68 bp), rs1059234 CT (three fragments of 183, 115 and 68 bp) and rs1059234 TT (one fragment of 183 bp). Right: A-D DNA sequencing—electropherograms corresponding to different genotypes. The polymorphic sites are indicated

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Table 1
Comparative analysis of genotype and allele distributions of the four polymorphisms, TP53 rs1042522 (G > C), TP53 rs17878362 (16 bp Del/Ins), p21 rs1801270 (C > A) and p21 rs1059234 (C > T), between the groups of cases and controls using different genetic models

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Table 2
Analysis of interaction between the TP53 rs1042522 (G > C) and TP53 rs17878362 (16 bp Del/Ins) polymorphisms, skin color/ ethnicity and development of SLE

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Table 3
Genotype interactions of the TP53 rs 1042522 (G>C), TP53 rs 17878362 (16 bp Del/Ins), p21 rs1801270 (C>A) and p21 rs 1059234 (C>T) polymorphisms between the group and subgroups of cases and controls stratified by skin color/ethnicity

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Table 4
Haplotype frequency estimation and haplotype association analysis, with respect to the TP53 polymorphisms, rs1042522 (G > C) and rs17878362 (16 bp Del/Ins), and the SNPs in the p21 (CDKN1A) gene, rs1801270 (C > A) and rs1059234 (C > T), in the entire study sample and in the groups stratified according skin color/ethnicity

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Table 5
Interaction analysis between the polymorphisms TP53 rs17878362 (16 bp Del/Ins) and TP53 rs1042522 (G > C) and clinical manifestations (serositis and neuropsychiatric disorders) of SLE patients

Polymorphism	Genotype/Allele	Controls^a a Controls—Hardy-Weinberg equilibrium test: TP53 rs1042522 (G > C) (p = 0.559); TP53 rs17878362 (16 bp Del/Ins) (p = 0.068); p21 rs1801270 (C > A) (p = 0.893); p21 rs1059234 (C > T) (p = 0.454) n (%) or n (f)	Cases^b b Cases—Hardy-Weinberg equilibrium test: TP53 rs1042522 (G > C) (p = 0.462); TP53 rs17878362 (16 bp Del/Ins) (p = 0.081); p21 rs1801270 (C > A) (p = 0.634); p21 rs1059234 (C > T) (p = 0.287) n (%) or n (f)	p value ^c c χ2 test or Fisher test.	Genetic model		Adjusted OR^d d Adjusted for age and skin color/ethnicity. p values > 0.05 (95% CI)
TP53 rs1042522 G > C	GG	64 (34.0)	37 (31.6)	0.6424	Codominant	GC vs. GG	1.21 (0.71-2.08)
	GC	88 (46.8)	61 (52.1)			CC vs. GG	1.09 (0.53-2.22)
	CC	36 (19.1)	19 (16.2)		Dominant	GC + CC vs. GG	1.18 (0.71-1.97)
	G	216 (0.57)	135 (0.58)	1.0000	Recessive	CC vs. GG + GC	0.97 (0.51-1.81)
	C	160 (0.43)	99 (0.42)		Overdominant	GC vs. GG + CC	1.18 (0.73-1.90)
TP53 rs17878362 16 bp Del/Ins	A1A1	136 (69.4)	77 (65.8)	0.7349	Codominant	A1A2 vs. A1A1	1.21 (0.70-2.07)
	A1A2	50 (25.5)	32 (27.4)			A2A2 vs. A1A1	1.44 (0.53-3.92)
	A2A2	10 (5.1)	8 (6.8)		Dominant	A1A2 + A2A2 vs.A1A1	1.25 (0.75-2.06)
	A1	322 (0.82)	186 (0.79)	0.4598	Recessive	A2A2 vs. A1A1 + A1A2	1.37 (0.51-3.67)
	A2	70 (0.18)	48 (0.21)		Overdominant	A1A2 vs. A1A1 + A2A2	1.17 (0.69-1.99)
p21 rs1801270 C > A	CC	103 (57.5)	83 (64.3)	0.3696	Codominant	CA vs. AA	0.86 (0.52-1.41)
	CA	66 (36.9)	42 (32.6)			AA vs. AA	0.54 (0.16-1.83)
	A/A	10 (5.6)	4 (3.1)		Dominant	CA+AA vs. CC	0.81 (0.50-1.32)
	C	272 (0.76)	208 (0.81)	0.2005	Recessive	AA vs. CC + CA	0.58 (0.17-1.91)
	A	86 (0.24)	50 (0.19)		Overdominant	CA vs. CC + AA	0.89 (0.55-1.46)
p21 rs1059234 C > T	CC	104 (61.5)	84 (65.6)	0.7948	Codominant	CT vs. CC	0.88 (0.52-1.47)
	CT	55 (32.5)	37 (28.9)			TT vs. CC	0.89 (0.32-2.46)
	TT	10 (5.9)	7 (5.5)		Dominant	CT+TT vs. CC	0.88 (0.54-1.43)
	C	263 (0.78)	205 (0.80)	0.5437	Recessive	TT vs. CC + CT	0.92 (0.34-2.54)
	T	75 (0.22)	51 (0.20)		Overdominant	CT vs. CC + TT	0.88 (0.53-1.48)

Polymorphism	Skin color/ethnicity	Genetic model	Controls n	Cases n	Adjusted OR (95% CI)^c c Adjusted for age
TP53 rs1042522 (G > C)^a a TP53 rs1042522 (G > C)—Allele frequencies: Whites—C versus G: OR 2.23; 95% CI 1.10-4.54; p = 0.037. Non-whites—C versus G: OR 0.85; 95% CI 0.57-1.26; p> 0.050	White	GG	18	12	1.00
		GC	14	25	2.73 (1.02-7.34) ^d d p = 0.041;
		CC	1	5	7.88 (0.80-77.25)
		GG	18	12	1.00
		GC + CC	15	30	3.06 (1.17-8.04) ^e e p = 0.021;
		GG + GC	32	37	1.00
		CC	1	5	4.43 (0.49-40.17)
		GG + CC	19	17	1.00
		GC	14	25	2.01 (0.80-5.080)
	Non-white	GG	45	25	1.00
		GC	74	36	0.85 (0.56-1.60)
		CC	35	14	0.72 (0.32-1.59)
		GG	45	25	1.00
		GC + CC	109	50	0.81 (0.45-1.47)
		GG + GC	119	61	1.00
		CC	35	14	0.79 (0.39-1.59)
		GG + CC	80	39	1.00
		GC	74	36	0.97 (0.55-69)
TP53 rs17878362 (16 bp Del/Ins)^b b TP53 rs17878362 (16 bp Del/Ins)—Allele frequencies: Whites—A2 versus A1: OR 7.00; 95% CI 1.99-24.66; p< 0.001. Non-whites—A2 versus A1: OR 0.83; 95% CI 0.51-1.37; p > 0.050	White	A1A1	30	25	1.00
		A1A2	3	13	5.22 (1.33-20.47) ^f f p = 0.003;
		A2A2	0	4	NA
		A1A1	30	25	1.00
		A1A2 + A2A2	3	17	6.93 (1.81-26.51) ^g g p = 0.001;
		A1A1 + A1A2	33	38	1.00
		A2A2	0	4	NA
		A1A1 + A2A2	30	29	1.00
		A1A2	3	13	4.47 (1.15-17.33) ^h h p = 0.018
	Non-white	A1A1	104	52	1.00
		A1A2	47	19	0.81 (0.43-1.52)
		A2A2	10	4	0.79 (0.24-2.64)
		A1A1	104	52	1.00
		A1A2 + A2A2	57	23	0.80 (0.45-1.45)
		A1A1 + A1A2	151	71	1.00
		A2A2	10	4	0.84 (0.25-2.77)
		A1A1 + A2A2	114	56	1.00
		A1A2	47	19	0.82 (0.44-1.54)

Genotype combination^a a Genotype combinations not represented in at least one group or subgroup are not shown Statistically significant results are in bold.				Total group			Whites			Non-whites
TP53 rs104252253 G >C	TP53 rs17878362 16 bp Del/Ins	p21 rs1801270 C > A	p21 rs1059234 C > T	Controls n	Cases n	OR (95% Cl)	Controls n	Cases n	OR (95% Cl)	Controls n	Cases n	OR (95% Cl)
GG	A1A1			63	36	1.00	18	12	1.00	44	24	1.00
GC	A1A1			55	39	1.24(0.70-2.22)	11	13	1.77 (0.60-5.25)	44	26	1.08(0.54-2.17)
GC	A1A2			30	22	1.28(0.65-2.55)	2	12	9.00 (1.70-47.62) ^b b p = 0.008;	28	10	0.65 (0.27-1.57)
GG		CC		36	22	1.00	9	10	1.00	27	12	1.00
GC		CC		44	38	1.41 (0.71-2.80)	9	15	1.50(0.44-5.10)	35	23	1.37(0.57-3.26)
GC		CA		30	16	0.87 (0.39-1.95)	3	7	2.10(0.41-10.67)	27	9	0.75 (0.27-2.07)
CC		CA		15	11	1.20(0.47-3.07)	1	3	2.70 (0.24-30.86)	14	8	1.29(0.43-3.88)
GG			CC	32	21	1.00	7	9	1.00	25	12	1.00
GG			CT	17	8	0.72 (0.26-1.96)	6	1	0.13 (0.01-1.34)	10	7	1.46 (0.44-4.78)
GC			CC	45	38	1.29(0.64-2.59)	9	15	1.30 (0.36-4.70)	36	23	1.33 (0.56-3.16)
GC			CT	25	17	1.04(0.45-2.37)	2	7	2.72 (0.42-17.43)	23	10	0.91 (0.33-2.49)
CC			CT	5	10	3.05(0.91-10.19)	1	1	0.78(0.04-14.76)	9	4	0.93 (0.24-3.62)
	A1A1	CC		66	52	1.00	16	19	1.00	50	33	1.00
	A1A1	CA		48	17	0.45 (0.23-0.87) ^c c p = 0.018;	10	3	0.25 (0.06-1.08)	36	14	0.59 (0.28-1.26)
	A1A2	CC		30	11	0.46(0.21-1.02)	3	6	1.68 (0.36-7.84)	27	5	0.28 (0.10-0.80) ^d d p = 0.015
	A1A1		CC	62	46	1.00	14	17	1.00	48	29	1.00
	A1A1		CT	40	19	0.64 (0.33-1.25)	9	5	0.46(0.12-1.68)	29	14	0.80 (0.36-1.76)
	A1A1		TT	6	5	1.12(0.32-3.91)	2	2	0.82 (0.10-6.62)	4	3	1.24(0.26-5.95)
	A1A2		CC	30	19	0.85 (0.43-1.70)	3	7	1.92 (0.42-8.84)	27	12	0.74 (0.32-1.67)
		CC	CC	89	68	1.00	16	25	1.00	73	43	1.00
		CC	CT	3	5	2.18(0.50-9.45)	1	2	1.28(0.11-15.31)	2	3	2.55(0.41-15.86)
		CA	CT	49	29	0.77 (0.44-1.35)	8	9	0.72 (0.23-2.25)	39	20	0.87 (0.45-1.68)

Haplotype	Total group			Whites			Non-whites
Haplotype	Controls (f)	Cases (f)	OR (95% CI)	Controls (f)	Cases (f)	OR (95% CI)	Controls (f)	Cases (f)	OR (95% CI)
TP53 rs17878362-rs1042522
A1-G	0.565	0.572	1.00	0.766	0.583	1.00	0.520	0.565	1.00
A1-C	0.255	0.223	0.85 (0.56-1.30)	0.203	0.167	1.40 (0.52-3.75)	0.268	0.255	0.88 (0.54-1.43)
A2-C	0.170	0.200	1.14 (0.75-1.71)	0.031	0.250	9.67 (2.02-46.28) ^a a p value: 0.006	0.200	0.172	0.81 (0.49-1.35)
A2-G	0.010	0.005	0.62 (0.09-4.22)	0	0	NA	0.013	0.008	0.69 (0.10-4.64)
Global haplotype association p value		0.69			< 0.001			0.83
p21 rs1801270-rs1059234
C-C	0.743	0.766	1.00	0.759	0.787	1.00	0.744	0.755	1.00
A-T	0.202	0.167	0.80 (0.51-1.24)	0.167	0.162	0.98 (0.39-2.49)	0.206	0.170	0.80 (0.47-1.35)
A-C	0.035	0.036	0.97 (0.37-2.52)	0	0.026	NA	0.042	0.041	0.94 (0.33-2.69)
C-T	0.019	0.031	1.49 (0.52-4.27)	0.074	0.026	0.42 (0.09-2.09)	0.008	0.034	4.46 (0.84-23.74)
Global haplotype association p value		0.65			0.34			0.23

Polymorphism	Genetic model	Serositis			Neuropsychiatric disorders
Polymorphism	Genetic model	Yes n	No n	OR (CI 95%)	Yes n	No n	OR (CI 95%)
TP53 rs17878362 16 bp Del/Ins	A1A1	35	39	1.00	13	61	1.00
	A1A2	21	10	2.34 (0.97-5.64)	8	24	1.56 (0.58-4.25)
	A2A2	0	8	NA	4	4	4.69 (1.04-21.24) ^b b p = 0.054;
	A1A1	35	39	1.00	13	61	1.00
	A1A2 + A2A2	21	18	1.30 (0.60-2.83)	12	28	2.01 (0.81-4.96)
	A2A2	0	8	1.00	4	4	1.00
	A1A1+ A1A2	56	49	NA	21	85	4.05 (0.93-17.53)
	A1A2	21	10	1.00	8	24	1.00
	A1A1 + A2A2	35	47	2.82 (1.18-6.74) ^a a p = 0.021;	17	65	1.27 (0.49-3.34)
	A1	91	88	1.00	34	146	1.00
	A2	21	26	0.78 (0.41-1.49)	16	32	2.15 (1.06-4.35) ^c c p = 0.048;
TP53 rs1042522 G > C	GG	19	18	1.00	4	32	1.00
	GC	31	26	1.13 (0.49-2.59)	13	46	2.26 (0.68-7.57)
	CC	6	13	0.44 (0.14-1.40)	8	11	5.82 (1.46-23.17) ^d d p = 0.015;
	GG	19	18	1.00	4	32	1.00
	GC + CC	37	39	0.90 (0.41-1.97)	21	57	2.95 (0.93-9.34)
	GG + GC	50	44	1.00	17	78	1.00
	CC	6	13	0.41 (0.14-1.16)	8	11	3.34 (1.17-9.55) ^e e p=0.031;
	GG + CC	25	31	1.00	12	43	1.00
	GC	31	26	1.48 (0.70-3.10)	13	46	1.01 (0.42-2.46)
	G	69	62	1.00	21	110	1.00
	C	43	52	0.74 (0.44-1.26)	29	68	2.23 (1.18-4.29) ^f f p = 0.015

[1] *Correspondence: Evandro Mendes Klumb klumb@uol.com.br

Brasil

Brasil

TP53 and p21 (CDKN1A) polymorphisms and the risk of systemic lupus erythematosus

Abstract

Background

Methods

Results

Conclusions

Highlights