The MelFo Study UK: Effects of a Reduced-Frequency, Stage-Adjusted Follow-Up Schedule for Cutaneous Melanoma 1B to 2C Patients After 3-Years

Moncrieff, Marc; Underwood, Beverly; Garioch, J.; Heaton, Martin; Patel, Nakul; Bastiaannet, E.; Hoekstra-Weebers, Josette E. H. M.; Hoekstra, Harald J.

doi:10.1245/s10434-020-08758-2

Cited by 16 publications

(24 citation statements)

References 33 publications

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“…Detailed methods of this multicentre, nonblinded, randomized clinical trial (ClinicalTrials.gov registration number: NCT01018004), initiated by the Department of Surgical Oncology at the University Medical Centre of Groningen (UMCG), have been described previously. [14][15][16] In summary, however, participants were randomized, in a 1:1 fashion, into 2 groups: one following the conventional schedule recommended in the current UK NICE or Dutch National melanoma guidelines, 17,18 and one whose follow-up was an AJCC stageadjusted reduced schedule (Table 1). Patients were stratified by country and AJCC stage (seventh edition), 19 in 2 random permuted blocks of 4 patients, generated by a validated system (Intrialgrator) with the use of a pseudorandom number generator and a supplied seed number.…”

Section: Methodsmentioning

confidence: 99%

“…Previously published results of the interim analysis of both studies at 3 years demonstrated the highly correlated data between the 2 countries. 14,15 After 5 years of follow-up, 240 (61.9%) completed and returned the PROMs questionnaires. The overwhelming majority ( > 97%) of patients remained satisfied with their follow-up schedule, regardless of the frequency of clinic visits.…”

Section: Quality Of Life and Patient-reported Outcome Measuresmentioning

confidence: 99%

“…The study was undertaken concurrently in the United Kingdom and the Netherlands, and the 3-year interim analyses concluded that the primary endpoints were not statistically different. 14,15 This final analysis addresses not only the primary endpoint at 5 years but also the predetermined intention of ultimately combining the international dataset to assess the secondary endpoints of detection rates and rate of recurrence in addition to survival outcomes (patient safety). The primary trial null hypothesis is that there is no difference in PROMs with a reduced-intensity AJCC stage-adjusted follow-up regimen when compared with the UK or Dutch national standard recommended follow-up regimen for AJCC pT1b-pT4bN0 melanoma patients staged with SNB.…”

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confidence: 99%

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Follow-up Schedule for Patients With Sentinel Node–negative Cutaneous Melanoma (The MELFO Study)

et al. 2022

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Objectives and Design: The MELFO (MELanoma FOllow-up) study is an international phase III randomized controlled trial comparing an experimental low-intensity schedule against current national guidelines. Background: Evidence-based guidelines for the follow-up of sentinel node–negative melanoma patients are lacking. Methods: Overall, 388 adult patients diagnosed with sentinel node–negative primary melanoma patients were randomized in cancer centers in the Netherlands and United Kingdom between 2006 and 2016. The conventional schedule group (control: n=196) was reviewed as per current national guidelines. The experimental schedule group (n=192) was reviewed in a reduced-frequency schedule. Quality of life was the primary outcome measurement. Detection rates and survival outcomes were recorded. Patient satisfaction rates and compliance with allocated schedules were compared. Results: At 5 years, both arms expressed high satisfaction with their regimens (>97%). This study found no significant group effect on any patient-reported outcome measure scores between the follow-up protocols. In total, 75/388 (19.4%) patients recurred, with no difference in incidence found between the 2 arms (hazard ratio=0.87, 95% confidence interval: 0.54–1.39, P=0.57). Self-examination was the method of detection for 25 experimental patients and 32 control patients (75.8% vs. 76.2%; P=0.41). This study found no difference in any survival outcomes between the 2 study arms (disease-free survival: hazard ratio=1.00, 95% confidence interval: 0.49–2.07, P=0.99). Conclusions: A reduced-intensity, American Joint Committee on Cancer (AJCC) stage-adjusted follow-up schedule for sentinel node–negative melanoma patients is a safe strategy, and patient self-examination is effective for recurrence detection with no evidence of diagnostic delay. Patients’ acceptance is very high.

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Section: Methodsmentioning

confidence: 99%

Section: Quality Of Life and Patient-reported Outcome Measuresmentioning

confidence: 99%

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confidence: 99%

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Follow-up Schedule for Patients With Sentinel Node–negative Cutaneous Melanoma (The MELFO Study)

et al. 2022

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“…Patients also incur travel and parking expenses, which may be especially burdensome for those who do not live close to the treatment centre. Fewer routinely scheduled clinic visits may have little impact on the detection of subsequent new primary or recurrent melanomas [12] and could result in substantial cost savings [13][14][15].…”

Section: Background and Rationale {6a}mentioning

confidence: 99%

Can Patient-Led Surveillance Detect Subsequent New Primary or Recurrent Melanomas and Reduce the Need for Routinely Scheduled Follow Up? A Protocol for the MEL-SELF Randomised Controlled Trial.

Ackermann

Smit

Janda

et al. 2021

Preprint

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Background: Most subsequent new primary or recurrent melanomas might be self-detected if patients are trained to systematically self-examine their skin and have access to timely medical review (patient-led surveillance). Routinely scheduled clinic visits (clinician-led surveillance) is resource-intensive and has not been shown to improve health outcomes; fewer visits may be possible if patient-led surveillance is shown to be safe and effective. The MEL-SELF trial is a randomised controlled trial comparing patient-led surveillance with clinician-led surveillance in people who have been previously treated for localised melanoma. Methods: Stage 0/I/II melanoma patients (n=600) from dermatology, surgical, or general practice clinics in NSW Australia, will be randomised (1:1) to the intervention (patient-led surveillance, n=300) or control (usual care, n=300). Patients in the intervention will undergo a second randomisation 1:1 to polarised (n=150) or non-polarised (n=150) dermatoscope. Patient-led surveillance comprises an educational booklet, skin self-examination (SSE) instructional videos; 3-monthly email/SMS reminders to perform SSE; patient-performed dermoscopy with teledermatologist feedback; clinical review of positive teledermoscopy through fast-tracked unscheduled clinic visits; and routinely scheduled clinic visits following each clinician’s usual practice. Clinician-led surveillance comprises an educational booklet and routinely scheduled clinic visits following each clinician’s usual practice. The primary outcome, measured at 12-months, is the proportion of participants diagnosed with a subsequent new primary or recurrent melanoma diagnosed at an unscheduled clinic visit. Secondary outcomes include time from randomisation to diagnosis (of a subsequent new primary or recurrent melanoma and of a new keratinocyte cancer), clinicopathological characteristics of subsequent new primary or recurrent melanomas (including AJCC stage), psychological outcomes, and healthcare use. A nested qualitative study will include interviews with patients and clinicians, and a costing study we will compare costs from a societal perspective. We will compare the technical performance of two different models of dermatoscope (polarised vs non-polarised).Discussion: The findings from this study may inform guidance on evidence-based follow up care, that maximises early detection of subsequent new primary or recurrent melanoma and patient wellbeing, while minimising costs to patients, health systems, and society.Trial registration: Australian New Zealand Clinical Trials Registry (ANZCTR): ACTRN12621000176864. Registered 18 February 2021, https://www.anzctr.org.au/ACTRN12621000176864.aspx

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“…Optimal follow-up surveillance strategies for patients who have been treated for primary melanoma by wide excision with or without SN biopsy have not been determined and are somewhat controversial, 9 but there are ongoing attempts to assemble evidence indicating the costeffectiveness of various follow-up schedules, notably the MELFO studies. 10,11 Although longer follow-up of these studies is required, results to date have shown that a less intensive follow-up schedule, with fewer clinic visits and less frequent routine imaging tests, did not adversely affect outcomes and substantially reduced costs for both patients and healthcare systems. Until now, there has been no information about the efficacy and cost of various followup surveillance strategies for melanoma patients who have had a positive SN but not a CLND, as in the experimental arms of both the MSLT-II and DeCOG-SLT studies.…”

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In Sentinel Node-Positive Melanoma Patients, Does Omission of Completion Lymph Node Dissection Make More Intensive Follow-Up Necessary, and Does Adjuvant Systemic Therapy Permit Less Intensive Follow-Up?

Thompson

2021

Ann Surg Oncol

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The MelFo Study UK: Effects of a Reduced-Frequency, Stage-Adjusted Follow-Up Schedule for Cutaneous Melanoma 1B to 2C Patients After 3-Years

Cited by 16 publications

References 33 publications

Follow-up Schedule for Patients With Sentinel Node–negative Cutaneous Melanoma (The MELFO Study)

Follow-up Schedule for Patients With Sentinel Node–negative Cutaneous Melanoma (The MELFO Study)

Can Patient-Led Surveillance Detect Subsequent New Primary or Recurrent Melanomas and Reduce the Need for Routinely Scheduled Follow Up? A Protocol for the MEL-SELF Randomised Controlled Trial.

In Sentinel Node-Positive Melanoma Patients, Does Omission of Completion Lymph Node Dissection Make More Intensive Follow-Up Necessary, and Does Adjuvant Systemic Therapy Permit Less Intensive Follow-Up?

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