Ignite Creation Date:
2024-10-26 @ 3:42 PM
Last Modification Date:
2024-10-26 @ 3:42 PM
Study NCT ID:
NCT06627036
Status:
NOT_YET_RECRUITING
Last Update Posted:
None
First Post:
2024-10-01
Brief Title:
Dermoscopy vs Standard Marking for the Completeness of Excision of Keratinocyte Skin Cancers The ClearMark Trial
Sponsor:
None
Organization:
None
Study Overview
Official Title:
Dermoscopy vs Standard Marking Practices for the Completeness of Excision of Keratinocyte Skin Cancers a Single-centre Randomised Controlled Trial
Status:
NOT_YET_RECRUITING
Status Verified Date:
2024-10
Last Known Status:
None
Delayed Posting:
No
If Stopped, Why?:
Not Stopped
Has Expanded Access:
No
If Expanded Access, NCT#:
N/A
Has Expanded Access, NCT# Status:
N/A
Acronym:
ClearMark
Brief Summary:
What is the study about This study aims to improve the success rate of removal surgery for a common type of skin cancer We will compare two different methods of marking drawing where to remove the skin before removing the lump the normal method using magnifying glasses and theatre lights and our proposed method using a handheld magnifying device called a dermatoscope
Why is this study important Skin cancer is the most common cancer in the UK Currently up to 10-11 of surgeries do not remove all of the cancer which means patients may need more treatment We do not know whether using a dermatoscope can help surgeons remove all of the cancer more often or not If it does it could prevent patients needing more surgery or time in hospital
What will happen during the study A computer will randomly allocate each participant to marking using the normal method or using a dermatoscope The surgery will then proceed as usual After the surgery patients will be asked to fill in a simple questionnaire about their thoughts We will collect data from patients notes to monitor the success of the surgery and any more treatments needed
What will we measure We will check participants records to see if the cancer was entirely removed This is reported by a pathologist whenever a skin lump or bump is removed In time we will also look at 5-year recurrence of cancer the need for additional treatments any problems from the marking process how happy patients are with the process and the time it takes to perform the marking
What is the pilot for The study will need many hundreds of patients to pick up a meaningful result Before we commit to recruiting this many people we want to make sure that the way we run the study is acceptable This means looking at the number of people we recruit each week how easy it is to collect their data after their operation and whether there are any areas that we cant use a dermatoscope such as the curves around the eye nose and ears We will run the study in a smaller number of people around 200 before deciding whether we can commit to recruiting everyone This will also give us the chance to see whether we can run the study in more than one hospital
Why is this study important Skin cancer is the most common cancer in the UK Currently up to 10-11 of surgeries do not remove all of the cancer which means patients may need more treatment We do not know whether using a dermatoscope can help surgeons remove all of the cancer more often or not If it does it could prevent patients needing more surgery or time in hospital
What will happen during the study A computer will randomly allocate each participant to marking using the normal method or using a dermatoscope The surgery will then proceed as usual After the surgery patients will be asked to fill in a simple questionnaire about their thoughts We will collect data from patients notes to monitor the success of the surgery and any more treatments needed
What will we measure We will check participants records to see if the cancer was entirely removed This is reported by a pathologist whenever a skin lump or bump is removed In time we will also look at 5-year recurrence of cancer the need for additional treatments any problems from the marking process how happy patients are with the process and the time it takes to perform the marking
What is the pilot for The study will need many hundreds of patients to pick up a meaningful result Before we commit to recruiting this many people we want to make sure that the way we run the study is acceptable This means looking at the number of people we recruit each week how easy it is to collect their data after their operation and whether there are any areas that we cant use a dermatoscope such as the curves around the eye nose and ears We will run the study in a smaller number of people around 200 before deciding whether we can commit to recruiting everyone This will also give us the chance to see whether we can run the study in more than one hospital
Detailed Description:
5 BACKGROUND AND RATIONALE 511 DESCRIPTION OF THE CONDITION Non-melanoma skin cancer NMSC also known as keratinocyte skin cancer KSC is the most prevalent cancer worldwide particularly affecting fair-skinned individuals who lack protective skin pigment In the United Kingdom UK the lifetime risk of developing keratinocyte skin cancer is 1 in 4 for men and 1 in 5 for women The two primary types of keratinocyte cancer are basal cell carcinoma BCC and cutaneous squamous cell carcinoma cSCC accounting for approximately 80 and 20 of cases respectively Other rare types of skin cancer such as Merkel cell carcinoma MCC and adenocarcinoma originating from skin gland cells each constitute about 02 to 04 of all NMSCs
BCCs generally develop after intense ultraviolet UV exposure during childhood and adolescence whereas cSCCs are associated with cumulative UV exposure and chronic sun damage The incidence of NMSC is rapidly increasing globally with the UK experiencing an 8 annual rise The incidence of cSCC appears to be growing faster than BCC particularly among elderly men who have accumulated substantial sun damage over their lifetimes This rise in incidence is primarily due to increased exposure to UV radiation both from the sun and artificial sources like tanning beds
Other significant risk factors for NMSC include advancing age male gender fair skin Fitzpatrick types I and II a history of skin cancer or severe sunburn immunosuppression family history of skin cancer and exposure to carcinogens such as arsenic and ionizing radiation However the true incidence of NMSC is uncertain due to underreporting and inconsistencies in registration practices In many countries NMSCs are not always documented and patients with multiple lesions may be registered only once leading to a potential underestimation of the actual burden
Despite their low mortality rates NMSCs cause significant morbidity and represent a growing economic burden on healthcare systems worldwide 3 They frequently appear on the head and neck where they can cause considerable local tissue destruction and disfigurement if treatment is inadequate or delayed While BCCs are generally localized and rarely metastasize cSCCs have the potential to spread to distant sites and become fatal
The typical presentation of NMSC includes ulcers nodules or scaly patches that do not heal and continue to grow at varying rates These lesions may bleed itch or cause significant local destruction BCCs predominantly arise on the head face and neck though some subtypes such as superficial BCCs are more common on the trunk and legs Conversely cSCCs typically occur on sun-exposed areas of the face such as the ears lips and scalp as well as on the neck shins and dorsum of the hands and forearms However both types can potentially develop anywhere on the body
512 DESCRIPTION OF DIAGNOSIS AND MANAGEMENT Patients who present to primary care with a suspicious skin lesion should be referred either routinely for suspected BCC or urgently to a two-week wait clinic for suspected SCC or BCC when there is concern that delay might significantly impact the patients prognosis These patients undergo a thorough assessment by a specialist either a dermatologist or a plastic surgeon This assessment includes a focused history and clinical examination dermoscopy and medical photography If the lesion is deemed suspicious the patient is scheduled for a biopsy-either excisional or incisional-to establish a histological diagnosis Management then depends on the biopsy results and for SCCs the TNM Tumour Node Metastasis staging guided by the Local Skin Multidisciplinary Team LSMDT or the Specialist Skin Cancer Multidisciplinary Team SSMDT
A comprehensive history and meticulous clinical examination are crucial for the accurate diagnosis of referred skin lesions Dermoscopy widely used by dermatologists and plastic surgeons is a non-invasive diagnostic tool for various skin lesions including skin cancer A dermatoscope is a handheld device that provides magnification from 10x to over 200x and has an adjustable built-in illumination system By transilluminating the lesion it visualises structures to the depth of the reticular dermis Modern dermatoscopes achieve this without additional translucency-enhancing solutions by using polarised light which filters out scattered light and allows visualisation of sub-stratal features Dermoscopy helps discriminate between different skin lesions based on color pattern and structural analysis When used by trained clinicians dermoscopy significantly improves the accuracy of skin cancer diagnosis for both melanoma and keratinocyte cancers It increases sensitivity for skin cancer detection decreases the benign-to-malignant biopsy ratio identifies cancers at an earlier stage and allows for the diagnosis of different BCC subtypes compared to naked eye examination NEE Dermatoscopic characteristics of lesions show good correlation with histopathological features of skin lesions making dermoscopy an invaluable part of the diagnostic approach to suspicious skin lesions
Once a lesion is inspected and deemed suspicious for skin cancer a biopsy is offered to confirm the diagnosis and assess risk The first-line treatment is often an excision biopsy where the entire lesion is removed with a margin of normal-appearing skin This approach aims to achieve complete excision and treatment without the need for further surgery or treatment Other biopsy options include incisional punch and shave biopsies which provide a smaller sample of the lesion for histopathological analysis Reconstruction if needed can be immediate or delayed based on the clarity of the clinical margins
The BAD has published guidelines based on studies using Mohs micrographic surgery MMS regarding recommended peripheral skin margins for BCCs and SCCs depending on clinical and pathological criteria that classify them as low high or very high only for SCCs risk For BCCs the recommended margins are 4-5mm for low-risk lesions and 5-10mm for high-risk lesions For SCCs the recommended margins are 4mm for low-risk 6mm for high-risk and 10mm for very high-risk lesions These margins are assessed preoperatively typically using theatre lights and loupe magnification as per BAD recommendations
Other treatment options include Mohs micrographic surgery especially for recurrent or poorly defined lesions in cosmetically sensitive areas electrodessication and curettage EDC cryosurgery radiotherapy RT photodynamic therapy PDT topical chemotherapy eg 5-fluorouracil and topical immunotherapy eg imiquimod Non-surgical methods lack histological confirmation of tumor clearance and are typically reserved for low-risk lesions with the exception of RT which is used routinely for older adults 60 with lesions of any risk category in well-vascularised anatomical sites who decline or are unsuitable for surgery
513 RATIONALE Skin cancer is the most prevalent cancer in the UK with a lifetime risk of 1 in 4 for men and 1 in 5 for women and an annual incidence increase of 8 The primary treatment approach involves complete surgical excision with UK dermatologists alone performing approximately 200000 NMSC excisions annually However incomplete excision rates vary ranging from 9 for squamous cell carcinomas to 11 for basal cell carcinomas This could mean up to 20000 patients annually that are inadequately treated Incomplete excision exacerbates morbidity imposing additional burdens such as the need for further surgeries or radiotherapy psychological distress productivity loss and increased costs for the NHS National Health Service These costs encompass theatre utilisation dressing materials consultant-led clinic appointments and prolonging already stretched waiting lists
The British Association of Dermatologists suggests a 95 complete excision rate as the gold standard when adhering to their guidelines for surgical marking indicating ample room for enhancement One way of potentially improving the rate of incomplete excision is by marking the lesion pre-excision with a dermatoscope - a handheld device providing high-factor magnification and polarised and non-polarised light specifically designed for the assessment of skin lesions Although dermoscopic marking of tumour margins shows promise evidence remains sparse Furthermore the use of dermoscopy for surgical margins vs common practices with theatre lights and loupes has not been formally compared with robust and high-quality prospective studies We are therefore proposing a study to evaluate the effectiveness of using dermoscopy for lesion marking prior to lesion excision Notably our inquiry has been identified as the second most crucial research question in skin cancer surgery by a James Lind Alliance JLA Priority Setting Partnership PSP By comparing standard practices using loupes and theatre lights with dermoscopy for preoperative marking of skin lesions we will therefore specifically help to address the PSP priority of What is the most effective way of determining the borders of the skin cancer before skin cancer surgery
514 OBJECTIVES To conduct a single-centre randomised controlled trial RCT comparing dermoscopy-guided excision with loupe-magnified excision in patients undergoing suspected keratinocyte cancer excision
BCCs generally develop after intense ultraviolet UV exposure during childhood and adolescence whereas cSCCs are associated with cumulative UV exposure and chronic sun damage The incidence of NMSC is rapidly increasing globally with the UK experiencing an 8 annual rise The incidence of cSCC appears to be growing faster than BCC particularly among elderly men who have accumulated substantial sun damage over their lifetimes This rise in incidence is primarily due to increased exposure to UV radiation both from the sun and artificial sources like tanning beds
Other significant risk factors for NMSC include advancing age male gender fair skin Fitzpatrick types I and II a history of skin cancer or severe sunburn immunosuppression family history of skin cancer and exposure to carcinogens such as arsenic and ionizing radiation However the true incidence of NMSC is uncertain due to underreporting and inconsistencies in registration practices In many countries NMSCs are not always documented and patients with multiple lesions may be registered only once leading to a potential underestimation of the actual burden
Despite their low mortality rates NMSCs cause significant morbidity and represent a growing economic burden on healthcare systems worldwide 3 They frequently appear on the head and neck where they can cause considerable local tissue destruction and disfigurement if treatment is inadequate or delayed While BCCs are generally localized and rarely metastasize cSCCs have the potential to spread to distant sites and become fatal
The typical presentation of NMSC includes ulcers nodules or scaly patches that do not heal and continue to grow at varying rates These lesions may bleed itch or cause significant local destruction BCCs predominantly arise on the head face and neck though some subtypes such as superficial BCCs are more common on the trunk and legs Conversely cSCCs typically occur on sun-exposed areas of the face such as the ears lips and scalp as well as on the neck shins and dorsum of the hands and forearms However both types can potentially develop anywhere on the body
512 DESCRIPTION OF DIAGNOSIS AND MANAGEMENT Patients who present to primary care with a suspicious skin lesion should be referred either routinely for suspected BCC or urgently to a two-week wait clinic for suspected SCC or BCC when there is concern that delay might significantly impact the patients prognosis These patients undergo a thorough assessment by a specialist either a dermatologist or a plastic surgeon This assessment includes a focused history and clinical examination dermoscopy and medical photography If the lesion is deemed suspicious the patient is scheduled for a biopsy-either excisional or incisional-to establish a histological diagnosis Management then depends on the biopsy results and for SCCs the TNM Tumour Node Metastasis staging guided by the Local Skin Multidisciplinary Team LSMDT or the Specialist Skin Cancer Multidisciplinary Team SSMDT
A comprehensive history and meticulous clinical examination are crucial for the accurate diagnosis of referred skin lesions Dermoscopy widely used by dermatologists and plastic surgeons is a non-invasive diagnostic tool for various skin lesions including skin cancer A dermatoscope is a handheld device that provides magnification from 10x to over 200x and has an adjustable built-in illumination system By transilluminating the lesion it visualises structures to the depth of the reticular dermis Modern dermatoscopes achieve this without additional translucency-enhancing solutions by using polarised light which filters out scattered light and allows visualisation of sub-stratal features Dermoscopy helps discriminate between different skin lesions based on color pattern and structural analysis When used by trained clinicians dermoscopy significantly improves the accuracy of skin cancer diagnosis for both melanoma and keratinocyte cancers It increases sensitivity for skin cancer detection decreases the benign-to-malignant biopsy ratio identifies cancers at an earlier stage and allows for the diagnosis of different BCC subtypes compared to naked eye examination NEE Dermatoscopic characteristics of lesions show good correlation with histopathological features of skin lesions making dermoscopy an invaluable part of the diagnostic approach to suspicious skin lesions
Once a lesion is inspected and deemed suspicious for skin cancer a biopsy is offered to confirm the diagnosis and assess risk The first-line treatment is often an excision biopsy where the entire lesion is removed with a margin of normal-appearing skin This approach aims to achieve complete excision and treatment without the need for further surgery or treatment Other biopsy options include incisional punch and shave biopsies which provide a smaller sample of the lesion for histopathological analysis Reconstruction if needed can be immediate or delayed based on the clarity of the clinical margins
The BAD has published guidelines based on studies using Mohs micrographic surgery MMS regarding recommended peripheral skin margins for BCCs and SCCs depending on clinical and pathological criteria that classify them as low high or very high only for SCCs risk For BCCs the recommended margins are 4-5mm for low-risk lesions and 5-10mm for high-risk lesions For SCCs the recommended margins are 4mm for low-risk 6mm for high-risk and 10mm for very high-risk lesions These margins are assessed preoperatively typically using theatre lights and loupe magnification as per BAD recommendations
Other treatment options include Mohs micrographic surgery especially for recurrent or poorly defined lesions in cosmetically sensitive areas electrodessication and curettage EDC cryosurgery radiotherapy RT photodynamic therapy PDT topical chemotherapy eg 5-fluorouracil and topical immunotherapy eg imiquimod Non-surgical methods lack histological confirmation of tumor clearance and are typically reserved for low-risk lesions with the exception of RT which is used routinely for older adults 60 with lesions of any risk category in well-vascularised anatomical sites who decline or are unsuitable for surgery
513 RATIONALE Skin cancer is the most prevalent cancer in the UK with a lifetime risk of 1 in 4 for men and 1 in 5 for women and an annual incidence increase of 8 The primary treatment approach involves complete surgical excision with UK dermatologists alone performing approximately 200000 NMSC excisions annually However incomplete excision rates vary ranging from 9 for squamous cell carcinomas to 11 for basal cell carcinomas This could mean up to 20000 patients annually that are inadequately treated Incomplete excision exacerbates morbidity imposing additional burdens such as the need for further surgeries or radiotherapy psychological distress productivity loss and increased costs for the NHS National Health Service These costs encompass theatre utilisation dressing materials consultant-led clinic appointments and prolonging already stretched waiting lists
The British Association of Dermatologists suggests a 95 complete excision rate as the gold standard when adhering to their guidelines for surgical marking indicating ample room for enhancement One way of potentially improving the rate of incomplete excision is by marking the lesion pre-excision with a dermatoscope - a handheld device providing high-factor magnification and polarised and non-polarised light specifically designed for the assessment of skin lesions Although dermoscopic marking of tumour margins shows promise evidence remains sparse Furthermore the use of dermoscopy for surgical margins vs common practices with theatre lights and loupes has not been formally compared with robust and high-quality prospective studies We are therefore proposing a study to evaluate the effectiveness of using dermoscopy for lesion marking prior to lesion excision Notably our inquiry has been identified as the second most crucial research question in skin cancer surgery by a James Lind Alliance JLA Priority Setting Partnership PSP By comparing standard practices using loupes and theatre lights with dermoscopy for preoperative marking of skin lesions we will therefore specifically help to address the PSP priority of What is the most effective way of determining the borders of the skin cancer before skin cancer surgery
514 OBJECTIVES To conduct a single-centre randomised controlled trial RCT comparing dermoscopy-guided excision with loupe-magnified excision in patients undergoing suspected keratinocyte cancer excision
Study Oversight
Has Oversight DMC:
None
Is a FDA Regulated Drug?:
None
Is a FDA Regulated Device?:
None
Is an Unapproved Device?:
None
Is a PPSD?:
None
Is a US Export?:
None
Is an FDA AA801 Violation?:
None