Editorial: Women in Hepato Pancreatic Biliary (HPB) Tumors: 2021, Volume I

The Research the diversity of research performed across the of by to and methodology, with applications to compelling problems related to pancreatic biliary

Also, STRING database (http://string-db.org) was utilized to construct PPI networks of coexpressed genes with interaction scores > 0.4. For visualization, CytoHubba, a plugin from the open-source platform Cytoscape (version 3.8.2) (http://www. cytoscape.org/), was employed to analyze and calculate the network structure.
Several concepts have been demonstrated or proved in the published articles (i) standard-of-care diagnostic biopsies and (ii) personalized therapy, and more.
HCC was addressed in 5 articles, while one presented colorectal cancer, however, pancreatic cancer was studied in 4 articles, by 89 authors.
The emerging importance of cancer personalized treatment plans is addressed in 3 research articles. As each human tumor creates its own unique microenvironment, He et al. claimed that assessment of BGN expression represents a promising approach for identifying patients with the greatest potential to benefit from immunotherapy and is a new venture into personalized therapy for colon cancer patients. BGN (a typical extracellular matrix (ECM) protein, validated as a signaling molecule regulating multiple processes of tumorigenesis), could serve as a valid biomarker for diagnosis, prognosis, and immunotherapy response prediction in patients with colon cancer.
Lundy et al.'s study demonstrates proof-of-principle feasibility to molecularly screen patients with pancreatic ductal adenocarcinoma for targeted therapies, and confirms diagnostic endoscopic ultrasound-guided fine-needle aspiration (EUS-FNA) biopsies. Single agent panitumumab was safe and tolerable but led to no objective tumor responses in the population tested.
In another study, Ren et al. revealed the clinicopathological features and identified risk factors of prognosis among patients with pancreatic cancer bone metastasis (PCBM), to be six independent predictors of prognosis, including age, pathological type, chemotherapy, liver metastasis, lung metastasis, and marital status. Knowledge of these survival predictors is helpful for clinicians to accelerate clinical decision process and design personalized treatment for patients with PCBM.
The crucial role of non-coding microRNAs (miRNAs) in pathogenesis of different diseases, including cachexia of strong pro-inflammatory environments, occurring in pancreatic and non-small cell lung cancer patients, was studied by Yehia et al. Where high levels of miR-155 in the cachectic group lead to negative feedback inhibition of both SOCS1 and the transcription factor Foxp3 in both the pancreatic and NSCL cancer patients.
Studies are also included on the roles of exosomes (Exo) in cancer development via mediating communication between tumor and its microenvironment. Hedgehog ligands undergo complicated post-translational modifications that result in lipid attachment and multimerization. Mutations in Hedgehog pathway components or induced Hedgehog signaling pathway components including Shh are found during injury or severe stress, or HBV or HCV infection and in HCC, as Li et al.'s group studied. They found higher plasma cancer cell-derived Exo-Shh levels associated with higher recurrence, suggesting Exo-Shh could serve as a prognostic biomarker and points to the possibility of tumor-secreted exosome being a therapeutic target.
As the demand for potential molecular biomarker(s) that can effectively predict prognosis and progression of HCC has increased, Ouyang et al. studied the anti-silencing function 1B (ASF1B) expression and function in HCC. They provided multilevel evidence for the significance of oncogenic gene ASF1B in HCC development and could be a target for inhibiting HCC cell growth, via inducing apoptosis and cell cycle arrest, reduced the expression of proliferating cell nuclear antigen (PCNA), cyclinB1, cyclinE2 and CDK9. These findings proposed a potential target for the development of anti-cancer strategies in HCC.
One of the major risk factors for HCC is hepatitis C virus (HCV) infection. The epithelial cell adhesion molecule (EpCAM) is a stem cell marker involved in the tumorigenesis and progression of many malignancies, including HCC, and was studied by Motawi et al. Serum EpCAM levels may hold promise for HCC diagnosis and for improving the diagnostic accuracy of a-fetoprotein.
Currently, there is a lack of tumor-selective and efficacious therapies for HCC. Zhao et al. studied the effect of the new chemotherapeutic agent b-Lapachone (b-lap; ARQ761 in clinical form) as a novel NADPH:quinone oxidoreductase 1 (NQO1) bioactivatable drug, selectively kills HCC cells expressing NQO1, through inducing ROS and PAR formation, NAD + and ATP depletion and lethal DNA damage. High NQO1:CAT ratios in HCC tumors but low ratios in normal tissues offer an optimal therapeutic window and an ideal therapeutic target for b-lap.
Jin et al. studied the role of response to antiviral therapies on survival of patients with intermediate-stage HBV-related HCC undergoing transarterial chemoembolization (TACE). They proved the importance of regular HBV DNA surveillance and durable viral suppression during antiviral treatment.
Finally, Bai et al. studied the combination of the well-tolerated modalities tumor treating fields (TTFields) with mild hyperthermia of 38.5°C, as a novel supporting therapy combination for pancreatic cancer, more effective than each single treatment, with greater efficacy results without increased toxicity.
Great potential and efforts in cancer prognosis and therapeutics still need to be worked on. Therefore, we still need to do more and more research for efficient predictive and prognostic molecularbiomarkers. Moreover, we still need to address (epi)genetic profiling for precision medicine implementation, and (epi)genetic new novel potential targets identification and characterization for cancer treatment and/or control. Let us move ahead with drug design and discovery as well as drug repurposing for HPB tumors, with special emphasis on nano-bio-medicine.

AUTHOR CONTRIBUTIONS
NMH was an associate editor of the Research Topic and wrote the paper text. YJ, SS, WW, YZ are guest associate editors for FIO and acted as editor for one paper in the Research Topic. BS was co-associate editor of the Research Topic. JC is a guest associate editor for FIO and acted as editor for two papers in the Research Topic. All authors contributed to the article and approved the submitted version.