HtrA1 in human urothelial bladder cancer: A secreted protein and a potential novel biomarker

Lorenzi, Teresa; Lorenzi, Maria; Altobelli, Emma; Marzioni, Daniela; Mensà, Emanuela; Quaranta, Alexia; Paolinelli, Francesca; Morroni, Manrico; Mazzucchelli, Roberta; Luca, Antonio De; Procopio, Antonio Domenico; Baldi, Alfonso; Muzzonigro, Giovanni; Montironi, Rodolfo; Castellucci, Mario

doi:10.1002/ijc.28280

Cited by 32 publications

(37 citation statements)

References 37 publications

(77 reference statements)

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“…S5D). This is consistent with previous studies that have shown the 38 kDa band is an autocatalytic product of the full length 50 kDa HtrA1 protein (28). Overall, SK-N-SH secreted HtrA1 protein levels were increased by 2.1-fold (p = 0.0002) after 9 days in culture with ATRA (Suppl.…”

Section: Introductionsupporting

confidence: 92%

The serine protease HtrA1 contributes to the formation of an extracellular 25-kDa apolipoprotein E fragment that stimulates neuritogenesis

Muñoz

Liu

Ruberu

et al. 2018

Journal of Biological Chemistry

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Apolipoprotein-E (apoE) is a glycoprotein highly expressed in the brain, where it appears to play a role in lipid transport, b-amyloid clearance, and neuronal signaling. ApoE proteolytic fragments are also present in the brain, but the enzymes responsible for apoE fragmentation are unknown, and the biological activity of specific apoE fragments remains to be determined. Here we utilised SK-N-SH neuroblastoma cells differentiated into neurons with all-trans retinoic acid (ATRA) to study extracellular apoE proteolysis. ApoE fragments were detectable in culture supernatants after 3 days, and their levels were increased for up to 9 days in the presence of ATRA. The concentration of apoE fragments was positively correlated with levels of the neuronal maturation markers (PSD95 and SMI32). The most abundant apoE fragments were 25 kDa and 28 kDa N-terminal fragments that both contained sialylated glycosylation and bound to heparin. We detected apoE fragments only in the extracellular milieu and not in cell lysates, suggesting that an extracellular protease contributes to apoE fragmentation.Of note, siRNA-mediated knockdown of high-temperature requirement serine peptidase A1 (HtrA1) and a specific HtrA1 inhibitor reduced apoE 25 kDa fragment formation by 41% and 86%, respectively. Recombinant 25-kDa fragment apoE and full-length apoE both stimulated neuritogenesis in vitro, increasing neuroblastoma neurite growth by more than 2-fold over a 6-day period. This study provides a cellular model for assessing apoE proteolysis, indicates that HtrA1 regulates apoE 25-kDa fragment formation under physiological conditions, and reveals a new neurotrophic function for the apoE 25-kDa fragment. ________________________________________

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Section: Introductionsupporting

confidence: 92%

The serine protease HtrA1 contributes to the formation of an extracellular 25-kDa apolipoprotein E fragment that stimulates neuritogenesis

Muñoz

Liu

Ruberu

et al. 2018

Journal of Biological Chemistry

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“…Therefore they proposed that the N-terminal domain may function as a redox-sensing element that regulates autoproteolytic activity of HtrA1 in vivo depending on the cellular redox state [114]. Their conclusion is closely connected to the earlier findings showing that HtrA1 undergoes a limited proteolytic processing [24,115,116]. Chien et al [24] demonstrated that in response to paclitaxel treatment of ovarian cancer cells HtrA1 underwent autocatalytic cleavage resulting in generation of the protease variant lacking the N-terminal domain.…”

Section: Structural Features Of Htra1mentioning

confidence: 71%

“…Although both the full-length HtrA1 and the processed form of the enzyme showed a similar proteolytic activity in vitro, the latter was more active in inducing apoptotic cell death [24]. The processed form of HtrA1 was observed in ovarian cell lines following anoikis-inducing conditions [15] and also in tumor tissues from patients with urothelial bladder cancer [116]. Apart from proving that redox changes influence HtrA1 cleavage in a cell, there still remains an open question, how HtrA1 lacking its N-terminal domain is regulated in vivo.…”

Section: Structural Features Of Htra1mentioning

confidence: 94%

Structural insights into the activation mechanisms of human HtrA serine proteases

Żurawa-Janicka

Wenta

Jarzab

et al. 2017

Archives of Biochemistry and Biophysics

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“…17,36 Recently, reduced levels of the autolytic ∼38 kDa product of HtrA1 were found to correlate with neoplastic bladder tissue undergoing cancerous transformation, which indeed highlights the importance of understanding the functional maturation of HtrA1 and the potential prognostic value of the autolytic forms. 28 …”

Section: Discussionmentioning

confidence: 99%

“…20,21 The specific downregulation of HtrA1 in the latter case promotes the sustained survival of cancer cells and the development of malignant metastatic behavior, 20,22,23 most likely correlated with the intracellular HtrA1 associated with microtubules and affecting cell migratory and signaling properties. 3,14,24−27 Interestingly, autolytically N-terminally truncated forms of HtrA1 exist in vivo , and such forms have been suggested as prognostic markers in urothelial bladder cancer 28 and in preeclamptic pregnancies. 18 The exact role and trigger of autolytic maturation is at present unknown.…”

mentioning

confidence: 99%

The Autolysis of Human HtrA1 Is Governed by the Redox State of Its N-Terminal Domain

et al. 2014

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Human HtrA1 (high-temperature requirement protein A1) belongs to a conserved family of serine proteases involved in protein quality control and cell fate. The homotrimeric ubiquitously expressed protease has chymotrypsin-like specificity and primarily targets hydrophobic stretches in selected or misfolded substrate proteins. In addition, the enzyme is capable of exerting autolytic activity by removing the N-terminal insulin-like growth factor binding protein (IGFBP)/Kazal-like tandem motif without affecting the protease activity. In this study, we have addressed the mechanism governing the autolytic activity and find that it depends on the integrity of the disulfide bonds in the N-terminal IGFBP/Kazal-like domain. The specificity of the autolytic cleavage reveals a strong preference for cysteine in the P1 position of HtrA1, explaining the lack of autolysis prior to disulfide reduction. Significantly, the disulfides were reduced by thioredoxin, suggesting that autolysis of HtrA1 in vivo is linked to the endogenous redox balance and that the N-terminal domain acts as a redox-sensing switch.

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HtrA1 in human urothelial bladder cancer: A secreted protein and a potential novel biomarker

Cited by 32 publications

References 37 publications

The serine protease HtrA1 contributes to the formation of an extracellular 25-kDa apolipoprotein E fragment that stimulates neuritogenesis

The serine protease HtrA1 contributes to the formation of an extracellular 25-kDa apolipoprotein E fragment that stimulates neuritogenesis

Structural insights into the activation mechanisms of human HtrA serine proteases

The Autolysis of Human HtrA1 Is Governed by the Redox State of Its N-Terminal Domain

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