Role of the IL8 rs4073 polymorphism in central nervous system toxicity in patients receiving multidrug-resistant tuberculosis treatment

Badamasi, Ibrahim Mohammed; Muhammad, Muktar; Umar, Aishat Ahmad; Madugu, Umm-ayman Misbahu; Gadanya, Muktar Ahmed; Aliyu, Isa Abubakar; Kabir, Imam Malik; Umar, Ibrahim Aliyu; Johnson, Ochigbo; Stanslas, Johnson

doi:10.36416/1806-3756/e20230338

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ORIGINAL ARTICLE • J. bras. pneumol. 50 (01) • 2024 • https://doi.org/10.36416/1806-3756/e20230338 copy

Role of the IL8 rs4073 polymorphism in central nervous system toxicity in patients receiving multidrug-resistant tuberculosis treatment

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Objective:

To determine the role of the IL8 rs4073 polymorphism in predicting the risk of central nervous system (CNS) toxicity in patients receiving standard pharmacological treatment for multidrug-resistant tuberculosis (MDR-TB).

Methods:

A cohort of 85 consenting MDR-TB patients receiving treatment with second-line antituberculosis drugs had their blood samples amplified for the IL8 (rs4073) gene and genotyped. All patients were clinically screened for evidence of treatment toxicity and categorized accordingly. Crude and adjusted associations were assessed.

Results:

The chief complaints fell into the following categories: CNS toxicity; gastrointestinal toxicity; skin toxicity; and eye and ear toxicities. Symptoms of gastrointestinal toxicity were reported by 59% of the patients, and symptoms of CNS toxicity were reported by 42.7%. With regard to the genotypes of IL8 (rs4073), the following were identified: AA, in 64 of the study participants; AT, in 7; and TT, in 11. A significant association was found between the dominant model of inheritance and CNS toxicity for the crude model (p = 0.024; OR = 3.57; 95% CI, 1.18-10.76) and the adjusted model (p = 0.031; OR = 3.92; 95% CI, 1.13-13.58). The AT+TT genotype of IL8 (rs4073) showed a 3.92 times increased risk of CNS toxicity when compared with the AA genotype.

Conclusions:

The AT+TT genotype has a tendency to be associated with an increased risk of adverse clinical features during MDR-TB treatment.

Keywords:
Tuberculosis, multidrug-resistant; Immunity; Pharmacogenetics; Polymerase chain reaction; Risk

Characteristic	MDR-TB patients receiving treatment (N = 82)
Age	31.88 ± 11.51
Sex (M/F)	54/28
Marital status (never married/once married)	41/41
Ethnicity (H/Y/I/O)	79/0/1/2
Religion (Islam/Christianity)	78/4
Job status(earning/dependent)	67/15
Family income (low income/high income)	74/8
Educational level (elementary/advanced)	66/16
Family history of tuberculosis (no/yes)	62/18
History of tuberculosis (no/yes)	59/23
History of tuberculosis treatment (no/yes)	72/10

Toxicity	Symptom	N (%)	With ADRs, n	Without ADRs, n
Gastrointestinal toxicity	Nausea/vomiting	25 (30.1%)	50	33
	Diarrhea	6 (7.2%)
	Constipation	2 (2.4%)
	Dry mouth	17 (20.5%)
Eye and ear toxicities	Blurred vision	6 (7.2%)	17	66
Eye and ear toxicities	Ringing in the ears	11 (13.3%)	17	66
Central nervous system toxicity	Headache	8 (9.8%)	35	47
	Tremors	12 (14.6%)
	Poor coordination	2 (2.4%)
	Dizziness	11 (11.0%)
Skin toxicity	Increased perspiration	2 (2.4%)	31	52
	Dry skin	10 (12.0%)
	Rash	9 (10.8%)
	Itching	10 (12.0%)

		CNS ADRs	No CNS ADRs	Crude estimate	Adjusted estimate
Codominant model	TT^a	7	4	-	-
	AA	23	41	p = 0.094; OR = 0.321 (95% CI, 0.085-1.212); R² _N = 0.088	p* = 0.070; OR = 0.26 (95% CI, 0.06-1.11); R² _N = 0.230
	AT	5	2	p = 0.733; OR = 1.429 (95% CI, 0.184-11.085); R² _N = 0.088	p = 0.959; OR = 1.063 (95% CI, 0.106-10.632); R² _N = 0.230
Overdominant model	AT	5	2	p* = 0.128; OR = 3.750 (95% CI, 0.683-20.602); R² _N = 0.042	p* = 0.240; OR = 3.24 (95% CI, 0.455-23.04); R² _N = 0.178
Overdominant model	AA+TT^a	30	45		p* = 0.240; OR = 3.24 (95% CI, 0.455-23.04); R² _N = 0.178
Dominant model	AA^a	23	41	p = 0.024; OR = 3.57 (95% CI, 1.18-10.76); R² _N = 0.086	p* = 0.031; OR = 3.92 (95% CI, 1.13-13.58); R² _N = 0.230
Dominant model	AT+TT	12	6	p = 0.024; OR = 3.57 (95% CI, 1.18-10.76); R² _N = 0.086	p* = 0.031; OR = 3.92 (95% CI, 1.13-13.58); R² _N = 0.230
Recessive model	AA+AT^a	28	43	p = 0.141; OR = 2.687 (95% CI, 0.720-10.035); R² _N = 0.036	p* = 0.097; OR = 3.350 (95% CI, 0.81-13.94); R² _N = 0.200
Recessive model	TT	7	4	p = 0.141; OR = 2.687 (95% CI, 0.720-10.035); R² _N = 0.036	p* = 0.097; OR = 3.350 (95% CI, 0.81-13.94); R² _N = 0.200

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[1] Correspondence to: Ibrahim Mohammed Badamasi. Pharmacogenomic Unit, Department of Human Anatomy, Faculty of Basic Medical Sciences - FBMS - College of Medicine, Bayero University, Kano, Kano State, Kano, Nigeria. Tel.: 08037024135. E-mail: bimohammed.ana@buk.edu.ng Johnson Stanslas. Pharmacotherapeutics Lab, Department of Medicine, Faculty of Medicine and Health Sciences, Universiti Putra Malaysia, Serdang, Malaysia. Tel.: 60 122670497. E-mail: jstanslas@yahoo.co.uk