Clinicopathological characteristics at primary melanoma diagnosis as risk factors for brain metastasis

Qian, Meng; Michelle, W.; Fleming, Nathaniel H.; Lackaye, Daniel J.; Hernando, Eva; Osman, Iman; Shao, Yongzhao

doi:10.1097/cmr.0000000000000015

Cited by 26 publications

(33 citation statements)

References 22 publications

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“…Prior retrospective studies of melanoma patients with BM examined cohorts ranging in size from 49 to 670 patients [5,6,8-12]. The rate of BM in these cohorts was approximately 10% [5,6,8,9,11,13], which corresponds to the expected risk of developing BM after a diagnosis of primary cutaneous melanoma [2].…”

Section: Discussionmentioning

confidence: 99%

“…The rate of BM in these cohorts was approximately 10% [5,6,8,9,11,13], which corresponds to the expected risk of developing BM after a diagnosis of primary cutaneous melanoma [2]. Our cohort of 123 melanoma patients with BM represented just over 2% of patients in our melanoma database; this lower percentage likely reflects the composition of our database, which contains many patients with melanoma in situ.…”

Section: Discussionmentioning

confidence: 99%

“…Previous studies examining factors predictive of melanoma BM have shown an association with depth and ulceration of the primary tumor as well as location on the head and neck [5,8-10]. In this study, along with analyzing additional patient demographic and primary tumor factors that may be associated with the development of BM, our aim was to investigate the impact of BM detection setting (routine screening vs. symptomatic presentation) on clinical outcomes.…”

Section: Introductionmentioning

confidence: 99%

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Risk factors for development of melanoma brain metastasis and disease progression: a single-center retrospective analysis

Gardner¹,

Ward

Andtbacka

et al. 2017

Melanoma Research

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Objective Melanoma metastasis to the brain is associated with poor prognosis. We sought to determine patient demographics and primary tumor factors associated with development of brain metastasis (BM) and survival. We also investigated whether the BM detection setting (routine screening vs. symptomatic presentation) affected clinical outcomes. Methods A database of melanoma patients seen from 1999-2015 at our institution was reviewed to identify patients that developed BM. Patients with BM were matched by initial stage with patients who did not develop BM as a control group. Patient demographics, primary tumor characteristics, and clinical outcomes were analyzed. Results 123 patients with BM were matched by initial presenting stage to 237 patients without BM. Characteristics of the primary melanoma tumor associated with BM development included location on the scalp (P=0.030), nodular histologic type (P=0.020) and Breslow depth >4mm (P=0.048), while location on the leg was associated with decreased BM risk (P=0.006). In patients with BM, time to first recurrence for melanomas of the scalp was significantly shorter (10.8 vs. 24.8 months, p=0.007) than non-scalp head and neck tumors. Patient stage, tumor depth, nodular type, and ulceration were also associated with worse clinical outcomes. There were no differences in clinical outcomes between patients whose BM were detected upon routine screening vs. upon symptomatic presentation. Conclusions Factors predictive of developing BM included primary scalp location, nodular type, and depth. In BM patients, scalp location, stage, tumor depth, nodular type and ulceration, but not detection setting, were associated with worse clinical outcomes.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Risk factors for development of melanoma brain metastasis and disease progression: a single-center retrospective analysis

Gardner¹,

Ward

Andtbacka

et al. 2017

Melanoma Research

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“…Another study by Baurain has shown the association of ulceration with clinical benefit of adjuvant vaccination with tumor-specific antigenic peptides in primary melanoma [41]. Ulceration has been known to be a histopathologic variable that portends increased metastatic risk [15, 42]. In this setting, ulceration may be more than a phenotype, but may in fact reflect, a more aggressive and immunogenic subtype of melanoma.…”

Section: Discussionmentioning

confidence: 99%

“…Work by Sarpa and colleagues demonstrated a significant relationship between the percentage of the tumor that is ulcerated and both sentinel lymph node status and OS; even minimal ulceration worsens the overall prognosis [14]. Moreover, ulceration, along with tumor thickness and disease stage, was shown to be one of the three risk factors most associated the development of brain metastasis [15]. …”

Section: Introductionmentioning

confidence: 99%

Immune biomarkers are more accurate in prediction of survival in ulcerated than in non-ulcerated primary melanomas

Moll

Qian

et al. 2015

Cancer Immunol Immunother

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Introduction Ulcerated melanomas may have a unique biology and microenvironment. We test whether markers of immune infiltration correlate with clinical outcome in ulcerated compared to non-ulcerated primary melanoma tumors. Methods Sixty-two stage II–III cutaneous melanomas, 32 ulcerated and 30 non-ulcerated, were analyzed for tumor-infiltrating lymphocytes (TILs). Immunohistochemistry (IHC) was performed for CD2, a marker previously shown to correlate with overall survival (OS) and recurrence-free survival (RFS) in this patient population. IHC using antibody, VE1, to BRAF V600E was also performed on a subset of 41 tumors to assess the relationship of BRAF mutation to immune markers. Results We found, using Cox regression models, that the presence of TILs was associated with improved OS (p = 0.034) and RFS (p = 0.002) in ulcerated melanoma tumors, but not in non-ulcerated melanoma (p = 0.632, 0.416). CD2 expression also was correlated with improved OS (p = 0.021) and RFS (p = 0.001) in ulcerated melanoma, but no relationship was seen in non-ulcerated melanoma (p = 0.427, 0.682). In this small population, BRAF status did not correlate with TILs or CD2+ count. Conclusion Our data show that immune markers including TILs and CD2 count correlate more closely with survival in ulcerated melanomas than that in non-ulcerated melanomas. We propose that immune biomarkers may be particularly relevant to ulcerated, as compared to non-ulcerated, melanomas and that this merits study in larger populations.

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High frequency of brain metastases after adjuvant therapy for high‐risk melanoma

et al. 2017

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The incidence of CNS progression in patients with high‐risk regional melanoma (stages IIIAN2a‐IIIC) is not well characterized. Data from the S0008 trial provided an opportunity to examine the role of CNS progression in treatment failure and survival. All patients were surgically staged. Following wide excision and full regional lymphadenectomy, patients were randomized to receive adjuvant biochemotherapy (BCT) or high‐dose interferon alfa‐2B (HDI). CNS progression was retrospectively identified from data forms. Survival was measured from date of CNS progression. A total of 402 eligible patients were included in the analysis (BCT: 199, HDI: 203). Median follow‐up (if alive) was over 7 years (range: 1 month to 11 years). The site of initial progression was identifiable in 80% of relapsing patients. CNS progression was a component of systemic melanoma relapse in 59/402 patients (15% overall). In 34/402 patients (9%) CNS progression represented the initial site of treatment failure. CNS progression was a component of initial progression in 27% of all patients whose melanoma relapsed (59/221). The risk of CNS progression was highest within 3 years of randomization. The difference in CNS progression rates between treatment arms was not significant (BCT = 25, HDI = 34, P = 0.24). Lymph node macrometastases strongly associated with CNS progression (P = 0.001), while ulceration and head and neck primaries were not significant predictors. This retrospective analysis of the S0008 trial identified a high brain metastasis rate (15%) in regionally advanced melanoma patients. Further studies are needed to establish whether screening plus earlier treatment would improve survival following CNS progression.

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Clinicopathological characteristics at primary melanoma diagnosis as risk factors for brain metastasis

Cited by 26 publications

References 22 publications

Risk factors for development of melanoma brain metastasis and disease progression: a single-center retrospective analysis

Risk factors for development of melanoma brain metastasis and disease progression: a single-center retrospective analysis

Immune biomarkers are more accurate in prediction of survival in ulcerated than in non-ulcerated primary melanomas

High frequency of brain metastases after adjuvant therapy for high‐risk melanoma

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