Literature summary for 3.4.21.20 extracted from

Shimoda, N.; Fukazawa, N.; Nonomura, K.; Fairchild, R.L.
Cathepsin G is required for sustained inflammation and tissue injury after reperfusion of ischemic kidneys (2007), Am. J. Pathol., 170, 930-940.

Search for more literature for 3.4.21.20

Protein Variants

Protein Variants	Comment	Organism
additional information	acute inflammatory response components are decreased by more than 50% in kidneys from cathepsin G-deficient versus wild-type mice, ischemic kidneys from cathepsin G-deficient mice have a 70% decrease in tubular cell apoptosis with little detectable collagen deposition, phenotypes, overview	Mus musculus

Natural Substrates/ Products (Substrates)

Natural Substrates	Organism	Comment (Nat. Sub.)	Natural Products	Comment (Nat. Pro.)	Rev.	Reac.
additional information	Mus musculus	cathepsin G as a critical component sustaining neutrophil-mediated acute tissue pathology and subsequent fibrosis after renal ischemia/reperfusion injury, cathepsin G is required for sustained inflammation and tissue injury after reperfusion of ischemic kidneys, overview	?	-	?

Organism

Organism	UniProt	Comment	Textmining
Mus musculus	-	129/SvJ wild-type mice	-

Source Tissue

Source Tissue	Comment	Organism	Textmining
kidney	healthy and ischemic	Mus musculus	-
neutrophil	synthesis and secretion	Mus musculus	-

Substrates and Products (Substrate)

Substrates	Comment Substrates	Organism	Products	Comment (Products)	Rev.	Reac.
additional information	cathepsin G as a critical component sustaining neutrophil-mediated acute tissue pathology and subsequent fibrosis after renal ischemia/reperfusion injury, cathepsin G is required for sustained inflammation and tissue injury after reperfusion of ischemic kidneys, overview	Mus musculus	?	-	?

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Release 2023.1 (January 2023)