Carboxypeptidase M in Brain and Peripheral Nerves

Nagae, Akihiro; Deddish, Peter A.; Becker, Robert P.; Anderson, Charles D.; Abe, Masahiro; Tan, Fulong; Skidgel, Randal A.; Erdös, Ervin G.

doi:10.1111/j.1471-4159.1992.tb10112.x

Cited by 45 publications

(8 citation statements)

References 49 publications

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“…B1R signaling was recently reported to prevent homing of encephalitogenic T-lymphocytes into the CNS, which was enhanced in B1R -/- mice 75. CPM, closely associated with myelin centrally and peripherally 76, should contribute by generating B1R ligands. The report mentioned that ACE inhibitor also suppresses inflammation in the CNS 75.…”

Section: Ace Inhibitors and Kinin Blrsmentioning

confidence: 96%

Angiotensin I–Converting Enzyme Inhibitors Are Allosteric Enhancers of Kinin B1 and B2 Receptor Function

2010

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Abstract-The beneficial effects of angiotensin I-converting enzyme (ACE) inhibitors go beyond the inhibition of ACE to decrease angiotensin (Ang) II or increase kinin levels. ACE inhibitors also affect kinin B1 and B2 receptor (B1R and B2R) signaling, which may underlie some of their therapeutic usefulness. Key Words: angiotensin I-converting enzyme inhibitors Ⅲ kininase II Ⅲ kinins Ⅲ bradykinin B2 receptor Ⅲ bradykinin B1 receptor Ⅲ allosteric regulation Ⅲ 7-transmembrane G protein-coupled receptor M illions of patients are treated with angiotensin I-converting enzyme (ACE) inhibitors to combat hypertension, congestive heart failure or diabetic renal diseases. 1-4 ACE inhibitors significantly reduce mortality after myocardial infarction 3 and are beneficial in other high risk patients.ACE inhibitors block the metabolism of several peptides by ACE, notably the conversion of angiotensin (Ang) I to II, 5 and the inactivation of bradykinin (BK) 6 -8 or the hemoregulatory tetrapeptide Ac-Ser-Asp-Lys-Pro. 9 The conversion of Ang I to Ang II was first found to occur in horse plasma 5 ; with kidney and human plasma, one of us reported the identity of ACE and kininase II, which we had discovered previously. 6 -8,10,11 Consequently, a single peptidyldipeptidase not only releases the hypertensive Ang II, but also inactivates the hypotensive BK. How much of the therapeutic effectiveness of ACE inhibitors is attributable to blocking Ang II release 12 or to prolonging the short half-life of BK 7 and its congener Lys1-BK (kallidin) has been debated. This is further complicated by the existence of 2 kinin receptors. The first characterized, but incongruously named, B2 receptor (B2R) is activated by native BK or kallidin. 13 The second, so-called B1 receptor (B1R), does not bind native kinins; its ligands are metabolites of BK and kallidin lacking the C-terminal arginine 14 removed by plasma carboxypeptidase (CP)N 15-17 or membrane CPM. 18 -20 Whereas the B2R is widely expressed constitutively, B1R expression is usually induced after noxious stimuli or by inflammatory cytokines, 13,14,[21][22][23] although some cells (bovine lung endothelial or human fibroblasts) express B1Rs constitutively.ACE inhibitors can enhance both B2 and B1R signaling. Blocking kinin inactivation by ACE raises the concentration of intact B2R agonists, which are also the substrates of CPN and -M. This can generate more des-Arg-kinin B1R agonists (Figure). The successful use of antagonists of the Ang II type 1 receptor (AT 1 R) for many of the same indications as ACE inhibitors does not prove ACE inhibitors work only through reducing Ang II as there are complex interrelationships among Ang II, BK and their receptors. Ang II has 2 receptors, AT 1 R and AT 2 R. AT 1 R is blocked by drugs such as losartan, which can shift Ang II actions to the AT 2 R. This switching of receptors further counteracts AT 1 R effects because it leads to the release of mediators such as nitric oxide (NO) and is attributed partially to release of BK to activate B2Rs, a form of "...

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Section: Ace Inhibitors and Kinin Blrsmentioning

confidence: 96%

Angiotensin I–Converting Enzyme Inhibitors Are Allosteric Enhancers of Kinin B1 and B2 Receptor Function

2010

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“…13,14 The highest levels of CPM have been found in human lung and placenta, but significant amounts are present in kidney, blood vessels, intestine, brain and in peripheral nerves. 2,13,15,16 CPM has been found in soluble form in various body fluids, including amniotic fluid, seminal plasma and urine. 3,17,18 Human CPM exhibits maximal proteolytic activity at neutral pH, contrasting with CPE or CPD, which have acidic pH optima.…”

Section: Introductionmentioning

confidence: 99%

Crystal Structure of Human Carboxypeptidase M, A Membrane-bound Enzyme that Regulates Peptide Hormone Activity

Reverter

Maskos

Tan

et al. 2004

Journal of Molecular Biology

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“…Bradykinin, anaphylatoxins, enkephalin hexapeptides, epidermal growth factor and dynorphin A have been reported to be naturally occurring substrates for CP-M. 33 The removal of the carboxy-terminal arginine or lysine results in the modification or inactivation of peptide hormone activity, and can also change the physical properties of the proteins. 35 CP-M has been reported to be distributed in organs and biological fluids such as the placenta, lungs, kidneys, intestines, brain, peripheral nerves, amniotic fluid and so on, 36 but there is no physiological role of CP-M in these tissues and fluids that has been clearly defined to date.…”

Section: Carboxypeptidase-m (Ec 341712)mentioning

confidence: 99%

Functional roles of cell surface peptidases in reproductive organs

Fujiwara

2004

Reprod Medicine & Biology

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A number of biologically active peptides have been proposed to regulate function and differentiation of reproductive organs in an autocrine and/or paracrine fashion. Regulation of the local concentrations of these peptides is one of the important factors influencing their physiological effects on target cells. Membrane-bound cell surface peptidases can activate or inactivate biologically active peptides before peptide factors access their receptors on the cell surface. Aminopeptidase A (EC 3.4.11.7), placental leucine aminopeptidase (EC 3.4.11.3), aminopeptidase-N/CD13 (EC 3.4.11.2), dipeptidyl peptidases IV/CD26 (EC.3.4.14.5), carboxypeptidase-M (EC 3.4.17.12), neutral endopeptidase/CD10 (EC 3.4.24.11) and endothelin converting enzyme-1 (EC 3.4.23) are differentially expressed on the ovary, endometrium and placenta. The inhibition of enzyme activity affects steroid hormone production by granulosa and thecal cells, decidualization of endometrium and migration of extravillous trophoblasts. These findings suggest that membrane-bound cell surface peptidases are local regulators for cellular growth and differentiation in reproductive organs by controlling extracellular concentration of peptide factors. (Reprod Med Biol 2004; : 165 -176).

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Carboxypeptidase M in Brain and Peripheral Nerves

Cited by 45 publications

References 49 publications

Angiotensin I–Converting Enzyme Inhibitors Are Allosteric Enhancers of Kinin B1 and B2 Receptor Function

Angiotensin I–Converting Enzyme Inhibitors Are Allosteric Enhancers of Kinin B1 and B2 Receptor Function

Crystal Structure of Human Carboxypeptidase M, A Membrane-bound Enzyme that Regulates Peptide Hormone Activity

Functional roles of cell surface peptidases in reproductive organs

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