The Serine Protease HtrA1 Is Upregulated in the Human Placenta during Pregnancy

Luca, Antonio De; Falco, Maria De; Fedele, Valentina; Cobellis, Luigi; Mastrogiacomo, Annunziata; Laforgia, Vincenza; Tuduce, Ioana L.; Campioni, Mara; Giraldi, D.; Paggi, Marco G.; Baldi, Alfonso

doi:10.1369/jhc.3a6186.2004

Cited by 52 publications

(55 citation statements)

References 44 publications

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“…A previous study reported the expression of HtrA1 during placental development in the human, but it focused on the transition from the first to the third trimester of pregnancy (De Luca et al, 2004). In the present study, we investigated the expression of HtrA1 mRNA and determined the cellular localization of HtrA1 protein during early placental development in the human.…”

Section: Introductionmentioning

confidence: 92%

Distinct expression and localization of serine protease HtrA1 in human endometrium and first‐trimester placenta

Nie¹,

Hale²,

Liu³

et al. 2006

Developmental Dynamics

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Mammalian embryos cannot survive without the placenta. Development of the human placenta requires trophoblast proliferation, differentiation, and invasion as well as highly coordinated modulation of the maternal uterus. HtrA1 is a member of the recently identified mammalian HtrA (high temperature requirement factor A) serine protease family with a high level of expression in the placenta. In this study, we examined whether HtrA1 expression (mRNA and protein) is associated with placental development in the human. HtrA1 is up-regulated in both endometrial glands and decidual cells during endometrial preparation for embryo implantation and during first-trimester pregnancy at placentation. HtrA1 expression was also detected in certain trophoblast subtypes during early pregnancy. The villous syncytiotrophoblast and cytotrophoblast showed the strongest expression while the interstitial extravillous trophoblast showed the lowest or no expression of HtrA1. The distinct distribution of HtrA1 at the maternaltrophoblast interface suggests that HtrA1 may play a role in placental development. Developmental Dynamics 235:3448 -3455, 2006.

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Section: Introductionmentioning

confidence: 92%

Distinct expression and localization of serine protease HtrA1 in human endometrium and first‐trimester placenta

Nie¹,

Hale²,

Liu³

et al. 2006

Developmental Dynamics

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“…Ubiquitously expressed in normal human adult tissues, 13 HtrA1 contains in addition to a highly conserved protease domain (trypsin like serine protease domain), an insulin growth factor-binding domain, a kazal type S protease inhibitor domain followed by one or two post-synaptic disclarge zona domains and a follistatin-like domain. 10 There is increasing evidences that HtrA1 regulates several physiological and pathological processes including tumour development, 14 Alzheimer's disease (AD), 15 placentation, 16 age-related macular degeneration 17 and osteoarthritis. 10 However, the mechanism(s) by which it regulates these processes has(ve) not been fully elucidated.…”

mentioning

confidence: 99%

“…10 However, the mechanism(s) by which it regulates these processes has(ve) not been fully elucidated. Considering its subcellular distribution, either found as a secreted protein or in the cytoplasm of the cells, 16 HtrA1 could act on different targets including extra-cellular matrix proteins. Interestingly, both HtrA1 and HtrA3 isoforms have been reported to inhibit TGF-b signalling during development 18,19 through a proteolyticallydependent interaction with ligands of the TGF-b family.…”

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confidence: 99%

HtrA1-dependent proteolysis of TGF-β controls both neuronal maturation and developmental survival

et al. 2008

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Transforming growth factor-b (TGF-b) signalling controls a number of cerebral functions and dysfunctions including synaptogenesis, amyloid-b accumulation, apoptosis and excitotoxicity. Using cultured cortical neurons prepared from either wild type or transgenic mice overexpressing a TGF-b-responsive luciferase reporter gene (SBE-Luc), we demonstrated a progressive loss of TGF-b signalling during neuronal maturation and survival. Moreover, we showed that neurons exhibit increasing amounts of the serine protease HtrA1 (high temperature responsive antigen 1) and corresponding cleavage products during both in vitro neuronal maturation and brain development. In parallel of its ability to promote degradation of TGF-b1, we demonstrated that blockage of the proteolytic activity of HtrA1 leads to a restoration of TGF-b signalling, subsequent overexpression of the serpin type -1 plasminogen activator inhibitor (PAI-1) and neuronal death. Altogether, we propose that the balance between HtrA1 and TGF-b could be one of the critical events controlling both neuronal maturation and developmental survival.

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“…Upregulation of HTRA1 was observed in endometrial glands and decidual cells during preparation of endometrium for embryo implantation and during the first trimester of placentation (Nie et al, 2006). However, the highest expression of HTRA1 was detected in placenta in the third trimester of gestation (De Luca et al, 2004). These data suggest an important role of HtrA1 in placenta development and function.…”

Section: Expressionmentioning

confidence: 82%