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Extended Abstract

Circulating Biochemical Molecular Markers (DNA and RNA) in Head and Neck Cancer: A Narrative Review †

Department of Oral and Maxillofacial Sciences, Sapienza University of Rome, 00161 Rome, Italy
*
Author to whom correspondence should be addressed.
Presented at the XV National and III International Congress of the Italian Society of Oral Pathology and Medicine (SIPMO), Bari, Italy, 17–19 October 2019.
Proceedings 2019, 35(1), 33; https://doi.org/10.3390/proceedings2019035033
Published: 10 December 2019
Head and neck cancers represent the sixth most common cancer group in humans [1]. Amongst these, head and neck squamous cell carcinoma (HNSCC) is the most frequent. In Europe the 5-year survival rate for HNSCC ranges from 25% to 60%, depending on primary tumor site and stage. The objective of a number of ongoing studies is to explore innovative techniques that allow early and reliable diagnosis and at the same time offer the possibility to monitor the evolution of the pathology.
The aim of this narrative review is to evaluate the role of biochemical molecular markers (liquid biopsy), such as DNA and RNA, in the diagnosis, prognostic outcome and treatment-monitoring in patients affected by HNSCC.
A selection of articles published until September 2019 on Pubmed formed the basis of the narrative review. The following inclusion and exclusion criteria were set: studies on human blood, plasma or serum evaluating DNA and RNA expression in patients with HNSCC compared to healthy controls (a minimum of 20 samples for each group needed); studies not including patients affected by Oral Squamous Cell Carcinoma (OSCC) were excluded. Amongst a total of 133 studies found, 8 met inclusion criteria (Figure 1).
Amongst all analysed studies, only one did not find a significant difference in the concentration of the circulating markers between the test group and the control group. Four studies evaluated the concentration of the circulating biochemical markers for the purpose of the diagnosis; one study for the prognostic outcome; one study for both diagnosis and treatment monitoring; two studies evaluated all three outcomes (Table 1).
Although liquid biopsy is an effective tool used by clinicians to approach other cancer types, such as Small Cell Lung Carcinoma (SCLC), its effectiveness with respect to HNSCC has to be investigated to a deeper extent. The biopsy therefore remains the gold standard in the diagnostic process of these cancers. However, liquid biopsy offers an advantage in the monitoring process of treated patients as it is less invasive when compared to Computed Tomography (CT) and Positron Emission Tomography (PET).
In the near future, biochemical molecular markers may lead the way to customized-patient therapy.

Conflicts of Interest

the authors declare no conflict of interest.

Reference

  1. Warnakulasuriya, S. Global epidemiology of oral and oropharyngeal cancer. Oral Oncol. 2009, 45, 309–316. [Google Scholar] [CrossRef] [PubMed]
Figure 1. Flow-chart of the selection process for studies included in the narrative review.
Figure 1. Flow-chart of the selection process for studies included in the narrative review.
Proceedings 35 00033 g001
Table 1. OSCC: Oral Squamous Cell Carcinoma; HSNCC: Head and Neck Squamous Cell Carcinoma; lncRNA: Long Noncoding RNA; cfDNA: Circulating Cell-Free DNA.
Table 1. OSCC: Oral Squamous Cell Carcinoma; HSNCC: Head and Neck Squamous Cell Carcinoma; lncRNA: Long Noncoding RNA; cfDNA: Circulating Cell-Free DNA.
First Author and Year Patients NumberTumor StageMatrixCell-Free Nucleic AcidDetection MethodAssesed for
Yang Li 2006OSCC: 32
Control: 35
Only Stage I and IISerummRNART-qPCRDiagnosis
Deepika Shukla 2013Potentially Malignant Lesions: 90
OSCC: 150 Post-Treatment
OSCC: 150 Control: 150
Not reportedBlood and PlasmacfDNANanoDrop spectrophotometerDiagnosis Treatment monitoring
Ya-Ching Lu 2015OSCC: 90
Pre-cancer: 16
Control: 53
I-II: 20
III-IV: 60
PlasmamiR-196a
miR-196b
RT-qPCRDiagnosis
Andreas Schröck 2017HSNCC: 421
Control: 224
Tis: 10 N0: 147
T1: 87 N1: 54
T2: 129 N2: 140
T3: 86 N3: 8
T4: 80 Nx: 72
NAd: 29
PlasmacfDNA (methylation)qPCRDiagnosis
Prognostic outcome
Treatment monitoring
Pooja Singh 2017OSCC: 20
OSMF: 20
Control: 40
Not reportedSerummiR-21RT-qPCRPrognostic outcome
Li-Han Lin 2018OSCC: 121
Control: 50
I-II: 40
III-IV: 81
PlasmacfDNAspectrophotometerDiagnosis
Prognostic outcome
Treatment monitoring
Tingru Shao 2018OSCC: 80
Control: 70
Not reportedSerumlncRNA
mRNA
RT-qPCRDiagnosis
Xinyuan Chen 2018HNSCC: 100
CONTROL: 100
I: 43
II: 31
III: 26
IV: 0
PlasmalncRNANanoDrop spectrophotometer (validation RT-qPCR)Diagnosis

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MDPI and ACS Style

Podda, G.M.; Rocchetti, F.; Pergolini, D.; Palaia, G.; Tenore, G.; Romeo, U. Circulating Biochemical Molecular Markers (DNA and RNA) in Head and Neck Cancer: A Narrative Review. Proceedings 2019, 35, 33. https://doi.org/10.3390/proceedings2019035033

AMA Style

Podda GM, Rocchetti F, Pergolini D, Palaia G, Tenore G, Romeo U. Circulating Biochemical Molecular Markers (DNA and RNA) in Head and Neck Cancer: A Narrative Review. Proceedings. 2019; 35(1):33. https://doi.org/10.3390/proceedings2019035033

Chicago/Turabian Style

Podda, Gian Marco, Federica Rocchetti, Daniele Pergolini, Gaspare Palaia, Gianluca Tenore, and Umberto Romeo. 2019. "Circulating Biochemical Molecular Markers (DNA and RNA) in Head and Neck Cancer: A Narrative Review" Proceedings 35, no. 1: 33. https://doi.org/10.3390/proceedings2019035033

APA Style

Podda, G. M., Rocchetti, F., Pergolini, D., Palaia, G., Tenore, G., & Romeo, U. (2019). Circulating Biochemical Molecular Markers (DNA and RNA) in Head and Neck Cancer: A Narrative Review. Proceedings, 35(1), 33. https://doi.org/10.3390/proceedings2019035033

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