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This version is not peer-reviewed
Submitted:
02 September 2024
Posted:
03 September 2024
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Diseases | Results | Pathological/Protective Role |
---|---|---|
Colon Cancer | High levels of MPO was observed in CRC tumors that can be considered as worse survival factor in patients [29]. | Pathological Role |
Breast Cancer | Penetration of MPO-positive cells is a new factor for improving survival of patients with breast cancer [20] | Protective Role |
Lung Cancer | Inhibition of MPO leads to reducing size and number of lung tumors and can be used as a protection agent of lung cancer [30] | Pathological Role |
Pancreatic Cancer | Increasing levels of NETs (such as MPO) are significantly related to tumor progression and malignancy of Pancreatic ductal adenocarcinoma [31] | Pathological role |
Arthrosclerosis | MPO contributes to arteriosclerosis by disrupting the function of endothelial cells, oxidation of LDL, and a high level of MPO is observed in all lesions of this disease [32]. | Pathological Role |
Myocardial Infarction | Reduced level of MPO and neutrophils is significantly contributed to decreased amount of myocardial infarction injury [33] | Pathological Role |
Heart Failure | Irreversible inhibition of MPO leads to reduced rate of heart failure injuries and also improving quality of life in patients with heart failure [34] | Pathological Role |
Alzheimer Disease | The increase in the adhesion of neutrophils and the amount of MPO caused by neutrophils causes vascular oxidative stress and can be one of the therapeutic goals of Alzheimer's disease [35]. | Pathological Role |
Multiple Sclerosis | Patients with multiple sclerosis have shown low serum levels of MPO, and low levels of MPO play an important role in the pathogenesis of this disease [36]. | Protective Role |
Parkinson Disease | High levels of MPO is observed in some brain areas related to this disease (such as putamen, caudate nucleus, and substantianigra) [37] | Pathological Role |
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Chang-Young Kim
et al.
,
2019
Michael Maes
et al.
,
2019
María Elena Soto
et al.
,
2024
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