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Research Articles

Inhibition of methotrexate induced toxicity in the adult rat spleen by adalimumab

, ORCID Icon, ORCID Icon, , , & show all
Pages 323-329 | Received 09 Sep 2021, Accepted 11 Jan 2022, Published online: 20 Jan 2022
 

Abstract

Methotrexate (MTX) has been in use for the treatment of rheumatoid arthritis (RA), psoriasis, and cancer since 1948. Its toxic side effects on tissues and organs have been well documented but splenotoxicity has not been addressed. This study set out to investigate this issue by examining the effectiveness of anti-TNFα agents against MTX-induced toxicity in T lymphocytes and macrophages via the regulation of CD3, CD68, and CD200R. Twenty-four Sprague Dawley rats were allocated to three groups: control (received saline solution only), MTX (20mg/kg of single-dose of MTX), and Ada + MTX (single dose of 10mg/kg Adalimumab before MTX administration). The spleens were removed 5days after MTX administration. The number of CD3+/mm3cells for the control, MTX and Ada + MTX groups were, respectively, 2.69±0.86, 20.51±2.7, (p=0.000) and 11.07±2.01 (p=0.000). The number of CD68+ macrophages/mm3 in the control, MTX and Ada + MTX groups were, respectively, 8.62±1.08, 38.19±1.37 (p=0.000), and 16.87±12.57 (p=0.000). The number of macrophages that were CD200R+/mm3 in the control, MTX, and Ada + MTX groups were 3.33±1.66, 25.77±2.37 (p=0.000), and 8.68±2.66 (p=0.000), respectively. We also observed that Ada reduced the numerical densities of these cells following MTX administration (p<0.05). Ada may, therefore, be a promising candidate for the prevention of the deleterious effects on T lymphocytes and macrophages of MTX-induced toxicity.

Acknowledgment

The authors received no financial support for the research, authorship, and/or publication of this article.

Author contributions

Concept & planning: IB, LT. Conduction of experiments: TM, OFD, NA, LT. Data analyses: IB, LT, TM, ZAY. Drafting of manuscript: All authors. Z.A.Y: Drafting, critical reading, translation and corrections.

Disclosure statement

No potential conflict of interest was reported by the author(s).

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