Pepsinogen C expression, regulation and its relationship with cancer

Shen, Shixuan; Jiang, Jingyi; Yuan, Yuan

doi:10.1186/s12935-017-0426-6

Cited by 30 publications

(22 citation statements)

References 81 publications

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“…Our previous results also indicated that the expression level of PGC gradually declined during SG‐AG‐GC progression 13. Melle et al14 also found that PGC was obviously reduced in gastric cancer tissue by ProteinChip Arrays and SELDI‐TOF MS. As a negative marker, PGC has demonstrated important value in the screening, diagnosis, and prognosis of gastric cancer 15, 16…”

Section: Introductionmentioning

confidence: 99%

Correlation between negative expression of pepsinogen C and a series of phenotypic markers of gastric cancer in different gastric diseases

et al. 2018

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Gastric tumorigenesis is a multistep process initiated by chronic superficial gastritis (SG), followed by atrophic gastritis (AG), then intestinal metaplasia (IM), and finally by dysplasia and adenocarcinoma according to the Correa model. Pepsinogen C (PGC) decreases gradually during progression of cancer, which makes PGC an ideal negative marker for GC. To explore the correlation between PGC and other positive tumor markers in different gastric diseases, we observed the expression of PGC, MG7‐Ag, MMP9, NM23, Ki‐67, and E‐cadherin by immunohistochemistry, quantitative RT‐PCR, and immunoblot analysis. Our results showed that in SG, PGC was highly expressed while malignant phenotype markers were rarely expressed. In contrast with SG, malignant phenotype markers were highly expressed while the positive rate of PGC reached only 1.44% in GC. So there was no coexpression of PGC and malignant phenotype markers in SG or GC tissues. Only in the AG group, which is well‐known to be gastric precancerous disease, coexpression of PGC and malignant phenotype markers was detected. Our results suggested that the expression of PGC in AG was negatively correlated with that of MG7‐Ag and MMP9. Of all AG, those with low expression of PGC and high expression of MG7‐Ag and MMP9 may possess a greater potential of malignant transformation. Combined detection of negative marker PGC and positive markers MG7‐Ag and MMP9 could be used as a potential follow‐up panel for monitoring dynamical progression of AG and improving the detection efficiency of high‐risk individuals of gastric cancer, and then taking necessary interventions on the target population.

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Section: Introductionmentioning

confidence: 99%

Correlation between negative expression of pepsinogen C and a series of phenotypic markers of gastric cancer in different gastric diseases

et al. 2018

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“…3d). Notably, the IM + CK organoids had significantly lower levels of SATB2 20 , Albumin (ALB), and Pepsinogen C (PGC) 39 expression compared with the CK + DCI HIOs (and IM + CHIR), suggesting that the IM + CK condition results in HIOs that are more homogenous and express markers specific to intestinal lineages, while preventing the emergence of hepatic and gastric lineages (Supplementary Fig. 3).…”

Section: Resultsmentioning

confidence: 99%

Generation of mesenchyme free intestinal organoids from human induced pluripotent stem cells

et al. 2020

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Efficient generation of human induced pluripotent stem cell (hiPSC)-derived human intestinal organoids (HIOs) would facilitate the development of in vitro models for a variety of diseases that affect the gastrointestinal tract, such as inflammatory bowel disease or Cystic Fibrosis. Here, we report a directed differentiation protocol for the generation of mesenchyme-free HIOs that can be primed towards more colonic or proximal intestinal lineages in serum-free defined conditions. Using a CDX2 eGFP iPSC knock-in reporter line to track the emergence of hindgut progenitors, we follow the kinetics of CDX2 expression throughout directed differentiation, enabling the purification of intestinal progenitors and robust generation of mesenchyme-free organoids expressing characteristic markers of small intestinal or colonic epithelium. We employ HIOs generated in this way to measure CFTR function using cystic fibrosis patient-derived iPSC lines before and after correction of the CFTR mutation, demonstrating their future potential for disease modeling and therapeutic screening applications.

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“…The advantage of this approach is that many different foreign domains may be fused to a target protein to increase its expression level or solubility and then be removed after expression in vivo, thereby allowing production of a target protein without any extra foreign domains. This strategy has been widely used for the production of many endogenous proteins, including growth factors and cytokines in animal cells as well as proteases such as pepsin and trypsin (Shi et al, 2011;Kim et al, 2011;Shen et al, 2017). These proteins are expressed as preproproteins and then converted to their functional form via proteolytic processing.…”

Section: Discussionmentioning

confidence: 99%

In Vivo Removal of N-Terminal Fusion Domains From Recombinant Target Proteins Produced in Nicotiana benthamiana

et al. 2020

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Plants show great potential for producing recombinant proteins in a cost-effective manner. Many strategies have therefore been employed to express high levels of recombinant proteins in plants. Although foreign domains are fused to target proteins for high expression or as an affinity tag for purification, the retention of foreign domains on a target protein may be undesirable, especially for biomedical purposes. Thus, their removal is often crucial at a certain time point after translation. Here, we developed a new strategy to produce target proteins without foreign domains. This involved in vivo removal of foreign domains fused to the N-terminus by the small ubiquitin-related modifier (SUMO) domain/SUMO-specific protease system. This strategy was tested successfully by generating a recombinant gene, BiP:p38:bdSUMO : His:hLIF, that produced human leukemia inhibitory factor (hLIF) fused to p38, a coat protein of the Turnip crinkle virus; the inclusion of p38 increased levels of protein expression. The recombinant protein was expressed at high levels in the leaf tissue of Nicotiana benthamiana. Coexpression of bdSENP1, a SUMO-specific protease, proteolytically released His:hLIF from the full-length recombinant protein in the endoplasmic reticulum of N. benthamiana leaf cells. His:hLIF was purified from leaf extracts via Ni 2+-NTA affinity purification resulting in a yield of 32.49 mg/kg, and the Nterminal 5-residues were verified by amino acid sequencing. Plant-produced His:hLIF was able to maintain the pluripotency of mouse embryonic stem cells. This technique thus provides a novel method of removing foreign domains from a target protein in planta.

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Pepsinogen C expression, regulation and its relationship with cancer

Cited by 30 publications

References 81 publications

Correlation between negative expression of pepsinogen C and a series of phenotypic markers of gastric cancer in different gastric diseases

Correlation between negative expression of pepsinogen C and a series of phenotypic markers of gastric cancer in different gastric diseases

Generation of mesenchyme free intestinal organoids from human induced pluripotent stem cells

In Vivo Removal of N-Terminal Fusion Domains From Recombinant Target Proteins Produced in Nicotiana benthamiana

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