Time patterns of recurrence and second primary tumors in a large cohort of patients treated for oral cavity cancer

Brands, Marieke T.; Smeekens, Elisabeth A. J.; Takes, Robert P.; Kaanders, Johannes H.A.M.; Verbeek, A.L.M.; Merkx, M.A.W.; Geurts, S.M.E.

doi:10.1002/cam4.2124

Cited by 45 publications

(37 citation statements)

References 40 publications

(90 reference statements)

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“…A cell identification tool to assist in the accurate and precise estimation of histopathological endpoints for the entire spectrum of OED and OSCC was developed. Figure shows the diagnostic categories and rates for oral cancer and dysplasia based on the World Health Organization classification found during mass screening, demonstrating 5‐year malignant transformations and 5‐year cancer recurrence rates . The literature presents a range of 5‐year transformation and recurrence rates, and we believe the ones listed herein are representative of those reported previously …”

Section: Resultssupporting

confidence: 54%

Point‐of‐care oral cytology tool for the screening and assessment of potentially malignant oral lesions

McRae

Modak

Simmons

et al. 2020

Cancer Cytopathology

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Background The effective detection and monitoring of potentially malignant oral lesions (PMOL) are critical to identifying early‐stage cancer and improving outcomes. In the current study, the authors described cytopathology tools, including machine learning algorithms, clinical algorithms, and test reports developed to assist pathologists and clinicians with PMOL evaluation. Methods Data were acquired from a multisite clinical validation study of 999 subjects with PMOLs and oral squamous cell carcinoma (OSCC) using a cytology‐on‐a‐chip approach. A machine learning model was trained to recognize and quantify the distributions of 4 cell phenotypes. A least absolute shrinkage and selection operator (lasso) logistic regression model was trained to distinguish PMOLs and cancer across a spectrum of histopathologic diagnoses ranging from benign, to increasing grades of oral epithelial dysplasia (OED), to OSCC using demographics, lesion characteristics, and cell phenotypes. Cytopathology software was developed to assist pathologists in reviewing brush cytology test results, including high‐content cell analyses, data visualization tools, and results reporting. Results Cell phenotypes were determined accurately through an automated cytological assay and machine learning approach (99.3% accuracy). Significant differences in cell phenotype distributions across diagnostic categories were found in 3 phenotypes (type 1 [“mature squamous”], type 2 [“small round”], and type 3 [“leukocytes”]). The clinical algorithms resulted in acceptable performance characteristics (area under the curve of 0.81 for benign vs mild dysplasia and 0.95 for benign vs malignancy). Conclusions These new cytopathology tools represent a practical solution for rapid PMOL assessment, with the potential to facilitate screening and longitudinal monitoring in primary, secondary, and tertiary clinical care settings.

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Section: Resultssupporting

confidence: 54%

Point‐of‐care oral cytology tool for the screening and assessment of potentially malignant oral lesions

McRae

Modak

Simmons

et al. 2020

Cancer Cytopathology

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“…The five year cumulative risk of a second event after surgical treatment of OC in a Dutch cohort of OSCC patients was assessed based on treatment type, previous malignancy, tumour location, whether the patient underwent a neck dissection, the presence of extracapsular spread and the presence of vaso-invasive growth. 12 Other authors have developed models to predict overall survival in OC and HNC patients based on clinical parameters such as WHO performance score, T-and N-stage, socioeconomic status score, age and gender, weight loss, BMI and smoking status. 20 Another way of personalizing follow-up is by selecting patients who will not have any curative treatment options left.…”

Section: Prediction Modelsmentioning

confidence: 99%

“…21 The parameters of this model are similar to the model developed in the Dutch cohort which predicted treatment in OC patients on the basis of tumour size, nodal status, previous treatment, invasion depth and ASA score. 12 These models will need further validation in other patient populations, but appear to be a useful instrument in selecting patients who may or may not benefit from routine follow-up.…”

Section: Prediction Modelsmentioning

confidence: 99%

“…5,10,11 The most important one being ending follow-up after two years as most recurrences occur within this timespan. 12,13 Furthermore, in practice, follow-up protocols are not strictly followed, as some clinicians apply a form of risk stratification based on patient-and tumour factors. 10,14 In addition, compliance to routine follow-up is expected to differ between patients.…”

Section: Introductionmentioning

confidence: 99%

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Follow‐up after oral cancer treatment—Transition to a personalized approach

Brands

Verbeek²,

Geurts

et al. 2021

J Oral Pathology Medicine

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After curative treatment for oral cancer (OC), patients enrol in a routine follow-up programme. Patients are at risk of a local or regional recurrence or a second primary tumour (SPT), even more so if they persist in their carcinogenic lifestyle.The main goal of routine follow-up is asymptomatic detection of new disease. 1 Other goals of follow-up are monitoring of treatment response, monitoring early-and late treatment morbidity and giving the patient and their loved ones psychological and emotional support. Routine follow-up is also used to evaluate medical treatment and quality of care with the aim to improve treatment for future patients and for training of doctors, nurses and paramedics. 2 The emphasis on the various goals might change over follow-up time. Soon after primary treatment, monitoring early side effects of the treatment will be more important, while later on the detection of SPT may have higher significance.

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“…Relapse for head and neck squamous cell carcinoma varies from 16% to 52% [2]. Patients with primary tumor diagnosis also have a higher chance to develop second primary tumors (SPTs), arising further than 2 cm from the primary site and/or 5 years later than primary diagnosis, due to an independent carcinogenesis leading to the onset of a new tumor [1,2]. Aim of the present study was to review retrospectively, from 2003 to 2018, how many patients, firstly diagnosed with an oral malignant neoplasm, experienced a subsequent malignant and/or premalignant disorder, in the form of new OPMD, cancerized OPMD, relapsed cancer or SPT.…”

Section: Introductionmentioning

confidence: 99%

Describing Clinical and Histological Outcome of Oral Cancer Patients with Recurrent Malignant or Premalignant Oral Lesions: A Retrospective Series with a Follow-Up of 15 Years

Cafaro

Cabras

Gambino

et al. 2019

The XV National and III International Congress of the Italian Society of Oral Pathology and Medicine

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Time patterns of recurrence and second primary tumors in a large cohort of patients treated for oral cavity cancer

Cited by 45 publications

References 40 publications

Point‐of‐care oral cytology tool for the screening and assessment of potentially malignant oral lesions

Point‐of‐care oral cytology tool for the screening and assessment of potentially malignant oral lesions

Follow‐up after oral cancer treatment—Transition to a personalized approach

Describing Clinical and Histological Outcome of Oral Cancer Patients with Recurrent Malignant or Premalignant Oral Lesions: A Retrospective Series with a Follow-Up of 15 Years

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