miR-21, miR-221, and miR-222 upregulation in lung cancer promotes metastasis by reducing oxidative stress and apoptosis

Tepebaşı, Muhammet Yusuf; Öztürk, Önder

doi:10.1590/1806-9282.20221688

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Brasil

Revista da Associação Médica Brasileira

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Original Article • Rev. Assoc. Med. Bras. 69 (6) • 2023 • https://doi.org/10.1590/1806-9282.20221688 copy

miR-21, miR-221, and miR-222 upregulation in lung cancer promotes metastasis by reducing oxidative stress and apoptosis

Authorship SCIMAGO INSTITUTIONS RANKINGS

SUMMARY

OBJECTIVE:

The purpose of our research was to observe the effects of miR-21, miR-221, and miR-222, as well as their target genes on oxidative stress, lung cancer formation, and metastasis.

METHODS:

Positron emission tomography/computed tomography, fiberoptic bronchoscopy, and/or endobronchial ultrasonography were performed on a total of 69 lung cancer patients to detect the presence or absence of metastasis, and the patients were classified based on the types of cancer. Total RNA and miRNA were isolated from the obtained biopsy samples. The quantitative analysis of hsa-miR-21-5p, hsa-miR-222-3p, and hsa-miR-221-3p and their target genes was performed by the RT-qPCR method. In determining oxidative stress, total antioxidant status and total oxidant status in tissue and total thiol and native thiol in blood were determined spectrophotometrically. OSI and disulfide were calculated.

RESULTS:

We discovered that the metastasis group had higher levels of hsa-miR-21-5p, hsa-miR-221-3p, and hsa-miR-222-3p (p<0.05). While TIMP3, PTEN, and apoptotic genes decreased in metastasis, anti-apoptotic genes increased (p<0.05). In addition, while oxidative stress decreased in the metastasis group, no change was found in the serum (p>0.05).

CONCLUSION:

Our findings show that upregulation of hsa-miR-21-5p, hsa-miR-221-3p, and hsa-miR-222-3p effectively contributes to both proliferation and invasion by influencing oxidative stress and mitochondrial apoptosis.

KEYWORDS:
Lung cancer; Metastasis; miRNA; Oxidative stress; Apoptosis

	Non-metastasis (n=32) Mean±SD [CI]	Metastasis (n=37) Mean±SD [CI]	p-value
hsa-miR-21-5p	1.17±0.65 [0.94–1.41]	3.80±1.57 [3.27–4.32]	<0.001^ p<0.001,
hsa-miR-221-3p	1.37±1.36 [0.88–1.85]	2.83±2.47 [2.00–3.65]	0.001^ p<0.001,
hsa-miR-222-3p	1.28±1.04 [0.90–1.65]	2.34±1.64 [1.81–2.90]	0.003^* * p<0.05.
TIMP3	1.43±1.11 [1.03–1.83]	0.66±0.50 [0.50–0.83]	0.002^* * p<0.05.
PTEN	1.24±0.81 [0.96–1.54]	0.49±0.28 [0.39–0.58]	<0.001^ p<0.001,
Caspase 9	1.40±1.15 [0.98–1.81]	0.34±0.29 [0.24–0.44]	<0.001^ p<0.001,
BAD	1.68±1.22 [1.24–2.12]	0.89±0.69 [0.66–1.12]	0.001^* * p<0.05.
BCL XL	1.52±1.31 [1.04–2.0]	4.49±2.44 [3.67–5.30]	<0.001^ p<0.001,
P53	1.62±1.36 [1.13–2.11]	0.90±0.76 [0.64–1.15]	0.015^* * p<0.05.
MDM2	1.26±1.03 [0.89–1.63]	3.75±3.08 [2.73–4.78]	<0.001^ p<0.001,

		Non-metastasis (n=32) Mean±SD [CI]	Metastasis (n=37) Mean±SD [CI]	p-value
TOS	Tissue	12.59±3.47 [11.34–13.84]	6.89±3.25 [5.8–7.9]	<0.001^ p<0.001.
TAS		1.63±1.67 [1.45–1.81]	1.67±0.36 [1.55–1.79]	0.694
OSI		0.84±0.36 [0.72–0.97]	0.42±0.21 [0.35–0.49]	<0.001^ p<0.001.
Total thiol	Serum	256.3±26.5 [247–266]	264.4±28.9 [258–278]	0.08
Native thiol		216.8±21.7 [209–225]	227.5±26.1 [219–236]	0.07
Disulfide		19.8±10.7 [15.9–23.6]	17.7±6.74 [15.4–19.9]	0.32

Non-metastasis and metastasis groups
	AUC	Cutoff	95%CI	Sensitivity %	Specificity %	p-value
hsa-miR-21-5p	0.979	>2.05	0.95–1.00	94.59	90.63	<0.001
hsa-miR-221-3p	0.733	>1.271	0.611–0.856	70.27	71.88	<0.001
hsa-miR-222-3p	0.707	>1.533	0.584–0.830	56.76	81.25	0.003

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[1] *Corresponding author: gultepe74@windowslive.com