TY - JOUR
T1 - Aberrant p16, p53 and Ki-67 immunohistochemistry staining patterns can distinguish solitary keratoacanthoma from cutaneous squamous cell carcinoma
AU - Carr, Richard A.
AU - Mesiano, Domenico
AU - Heffron, Cynthia
AU - Radonic, Teodora
AU - Wiggins, James
AU - Tso, Simon
AU - Agrawal, Rishi
AU - Cheung, Elaine
AU - Slater, David N.
AU - Nichols, Linda
AU - Craig, Paul
N1 - Funding Information: Charlotte Proby, Dermatology, Ninewells Hospital and Medical School, Dundee, UK, Eugene Healy, Dermatology, Southampton, UK, and Neil Catterall, Consultant Anatomical Pathologist, Laverty Pathology, Newcastle, NSW, Australia, for kindly discussing the work, reading the manuscript and making editorial suggestions. Luis Caballero Requena, Prof of Dermatology, University of Madrid, Spain for reading the manuscript and providing highly positive feedback. Saleem Taibjee, Consultant Dermatologist and Dermatopathologist, Dorchester, UK, and Zuliatul Faizah, Histopathologist, Hospital Kuala Lumpur, Malaysia, for attending the consensus meeting and contributions to discussions in the early stages of the proposed audit. Colleagues Scott Sanders, Sixto Baiting, Amgad Youssef in the skin reporting team, Warwick Hospital, UK, who adopted regular use of immunostaining and EVG in the work-up of cases of cSCC and KA. Publisher Copyright: © 2023
PY - 2023/10
Y1 - 2023/10
N2 - Keratoacanthoma (KA) is widely considered a benign, usually self-resolving, neoplasm distinct from cutaneous squamous cell carcinoma (cSCC), while some consider KA to be indistinguishable from cSCC. Published studies indicate utility for p16, p53, Ki-67 immunostaining and elastic van Gieson (EVG) in the assessment of KA and cSCC. We compared clinical features and staining patterns for p16, p53, Ki-67 and EVG in fully excised KA, cSCC with KA-like features (cSCC-KAL) and other cSCC (cSCC-OTHER). Significant differences between KA, cSCC-KAL and cSCC-OTHER were found for head and neck location (20%, 86%, 84%), and duration <5 months (95%, 63%, 36%). KA shows both a mosaic pattern for p16 (>25–90% of neoplasm area) and peripheral graded pattern for p53 (up to 50% moderate and strong nuclear staining) in 92% compared with 0% of cSCC-KAL and 0% of cSCC-OTHER. In contrast, a highly aberrant pattern (usually null) for one or both p16 and p53, was present in 0% of KA, 83.8% of cSCC-KAL and 90.9% of cSCC-OTHER. Abnormal distribution of Ki-67 beyond the peripheral 1–3 cells was uncommon in KA (4.2%) and common in cSCC-KAL (67.6%) and cSCC-OTHER (88.4%). Moderate to striking entrapment of elastic and collagen fibres was present in the majority of KA (84%), cSCC-KAL (81%) and cSCC-OTHER (65%). KA are clinically distinct neoplasms typically of short duration occurring preferentially outside the head and neck and generally lacking aberrations of p16, p53 and Ki-67, compared with cSCC that have high rates of aberrant or highly aberrant p16, p53 and Ki-67, but EVG lacked specificity.
AB - Keratoacanthoma (KA) is widely considered a benign, usually self-resolving, neoplasm distinct from cutaneous squamous cell carcinoma (cSCC), while some consider KA to be indistinguishable from cSCC. Published studies indicate utility for p16, p53, Ki-67 immunostaining and elastic van Gieson (EVG) in the assessment of KA and cSCC. We compared clinical features and staining patterns for p16, p53, Ki-67 and EVG in fully excised KA, cSCC with KA-like features (cSCC-KAL) and other cSCC (cSCC-OTHER). Significant differences between KA, cSCC-KAL and cSCC-OTHER were found for head and neck location (20%, 86%, 84%), and duration <5 months (95%, 63%, 36%). KA shows both a mosaic pattern for p16 (>25–90% of neoplasm area) and peripheral graded pattern for p53 (up to 50% moderate and strong nuclear staining) in 92% compared with 0% of cSCC-KAL and 0% of cSCC-OTHER. In contrast, a highly aberrant pattern (usually null) for one or both p16 and p53, was present in 0% of KA, 83.8% of cSCC-KAL and 90.9% of cSCC-OTHER. Abnormal distribution of Ki-67 beyond the peripheral 1–3 cells was uncommon in KA (4.2%) and common in cSCC-KAL (67.6%) and cSCC-OTHER (88.4%). Moderate to striking entrapment of elastic and collagen fibres was present in the majority of KA (84%), cSCC-KAL (81%) and cSCC-OTHER (65%). KA are clinically distinct neoplasms typically of short duration occurring preferentially outside the head and neck and generally lacking aberrations of p16, p53 and Ki-67, compared with cSCC that have high rates of aberrant or highly aberrant p16, p53 and Ki-67, but EVG lacked specificity.
KW - CDNK2A
KW - Keratoacanthoma
KW - Ki-67
KW - cutaneous squamous cell carcinoma
KW - elastic van Gieson
KW - p16
KW - p53
UR - http://www.scopus.com/inward/record.url?scp=85168392217&partnerID=8YFLogxK
U2 - https://doi.org/10.1016/j.pathol.2023.07.001
DO - https://doi.org/10.1016/j.pathol.2023.07.001
M3 - Article
C2 - 37573161
SN - 0031-3025
VL - 55
SP - 772
EP - 784
JO - Pathology
JF - Pathology
IS - 6
ER -