Extracellular Domain of IL-10 Receptor Chain-2 (IL-10R2) and Its Arginine-Containing Peptides Are Susceptible Substrates for Human Prostate Kallikrein-2 (KLK2).
Juliana R OliveiraJosé Thalles LacerdaTarciso A SellaniElaine G RodriguesLuiz R TravassosMaria A JulianoLuiz JulianoPublished in: Biochemistry (2024)
The kallikrein-related peptidase KLK2 has restricted expression in the prostate luminal epithelium, and its protein target is unknown. The present work reports the hydrolytic activities of KLK2 on libraries of fluorescence resonance energy-transfer peptides from which the sequence SYRIF was the most susceptible substrate for KLK2. The sequence SYRIF is present at the extracellular N -terminal segment ( 58 SYRIF 63 Q) of IL-10R2. KLK2 was fully active at pH 8.0-8.2, found only in prostate inflammatory conditions, and strongly activated by sodium citrate and glycosaminoglycans, the quantities and structures controlled by prostate cells. Bone-marrow-derived macrophages (BMDM) have IL-10R2 expressed on the cell surface, which is significantly reduced after KLK2 treatment, as determined by flow cytometry (FACS analysis). The IL-10 inhibition of the inflammatory response to LPS/IFN-γ in BMDM cells due to decreased nitric oxide, TNF-α, and IL-12 p40 levels is significantly reduced upon treatment of these cells with KLK2. Similar experiments with KLK3 did not show these effects. These observations indicate that KLK2 proteolytic activity plays a role in prostate inflammation and makes KLK2 a promising target for prostatitis treatment.
Keyphrases
- prostate cancer
- energy transfer
- induced apoptosis
- nitric oxide
- benign prostatic hyperplasia
- oxidative stress
- amino acid
- cell cycle arrest
- rheumatoid arthritis
- poor prognosis
- cell surface
- endothelial cells
- immune response
- mesenchymal stem cells
- signaling pathway
- combination therapy
- emergency department
- hydrogen peroxide
- cell proliferation
- bone marrow
- long non coding rna
- pi k akt
- adverse drug
- drug induced
- replacement therapy