Prognostic Factors in Malignant Melanoma

Bolander, Åsa

January 2008

Because of the failure so far to find effective treatment for patients with advanced stages of melanoma, increasing efforts have been made to find prognostic factors identifying patients in the risk zone for development of metastasis. This thesis investigates the prognostic powers of a few selected serological and immunohistochemical biomarkers. In the first and second study, patients operated on for localized malignant melanoma were investigated regarding the prognostic impact of angiogenic serological markers and circulating levels of S100. We concluded that the S100 assays, especially S100BB, are potential biomarkers in patients with malignant melanoma, correlated to both survival and disease free survival. However, no such conclusion could be drawn from the first study, where we found no correlation to survival and investigated angiogenic markers. In the third and fourth study four new potential immunohistochemical biomarkers where investigated in collaboration with the Swedish Human Protein Atlas Program, and those where TRP-1, galectin-1, DLG5 and syntaxin-7. We found that TRP-1 correlated inversely with tumor stage and galectin-1 correlated to Ki-67. DLG5 showed a significant inverse correlation to Ki67 and the expression of STX7 was inversely correlated to tumor stage, suggesting that decreased expression is associated with more aggressive tumors. None of the investigated markers in study III and IV correlated with disease free survival or overall survival. In the fifth and last study, we examined the expression of SOX10, a transcription factor, in different melanocytic lesions. Also, a proliferation assay was carried out in a human melanoma cell line. The results reveal the presence of SOX10 in different melanocytic lesions, with a weak inverse correlation to survival and a significant inverse correlation to T-stage. A significant decrease in proliferation rate for SOX10 silenced cells was found and our data also suggests an increased migratory response in SOX10 silenced cells.

Malignant melanoma

prognostic factors

survival

chemotherapy

radiation

SIMULTANEOUS SURGICAL RESECTIONS OF TWO DISTANT METASTATIC MALIGNANT MELANOMA LESIONS : CASE REPORT

WAKABAYASHI, TOSHIHIKO, HIRANO, MASAKI, TAKEBAYASHI, SHIGENORI, NAKAHARA, NORIMOTO, TANEI, TAKAFUMI

02 1900

No description available.

Metastatic

Surgical resection

Simultaneous

Multiple

Malignant melanoma

Adoptive T Cell Therapy for Treatment of Metastatic Melanoma

Sadeghi, Arian

January 2011

Malignant melanoma is a common type of solid tumor that causes high cancer-related mortality in young adults of Northern Europe. The incidence of melanoma increases rapidly which renders us a special responsibility to investigate this disease in depth. One recent promising approach to treat malignant melanoma is adoptive cell therapy with tumor-directed autologous T cells. This thesis aims to improve this therapy in four different studies. We first sought to establish a protocol for the assessment of melanoma-specific T-cell cultures in order to screen for optimal specificity and reactivity in a robust, reliable and simple manner. The conclusion was that reactive cells could be found in a majority of patients and could be screened for specificity by stimulation with melanoma cell lines. In the next study, 28 melanoma patients with advanced disease were treated with autologous tumor-infiltrating T cells. Objective responses (18%) including one sustained complete response were observed. This is the first study in cancer patients with autologous T cell transfer combined with low-dose s.c. IL-2 as supportive cytokine. In the following two studies we wanted to improve management and culture conditions of the T cells. When investigating methods for improved handling and preservation of large numbers of T cells, we observed that freeze-thawing of T cells could impair the metabolic activity of the T cells. Another conclusion was that rapid expansion of T cells could lead to loss of antigenic specificity and apoptosis. These adverse effects could be prevented with short time recovery. In order to improve expansion methods, mass expansion of T cells in an automated bioreactor was evaluated. We concluded that the bioreactor is suitable for this task and allows for higher cell densities and absolute cell numbers compared to traditional culturing conditions without influencing cell phenotype or reactivity. Taken together, my current studies present guiding principles and encouragement for the further development of immunotherapies for treatment of patients with malignant melanoma.

Malignant melanoma

Adoptive cell therapy

MEDICINE

MEDICIN

Creation, Delivery, and Evaluation of a Malignant Melanoma Continuing Education Program for Pharmacists

Cooley, Janet, Gunderson, Lisa, Tate, Jacqueline

January 2006

Class of 2006 Abstract / Objectives: To create, deliver, and evaluate a malignant melanoma continuing education (CE) seminar for pharmacists. Methods: A CE program was developed and presented to educate pharmacists about skin cancer prevention, specifically malignant melanoma, and their role in prevention through patient counseling. All practicing pharmacists who attended the CE program were asked to fill out a knowledge indicator and assess their comfort level in counseling patients about sun safety before and after the program. The participants also answered questions addressing how often they counsel patients on sunscreen use, their personal experience with skin cancer, preferred CE format, previous CE attendance, sex, age, practice site, hours worked per week, and years since graduation from pharmacy school. Results: The survey instrument was completed by 84 pharmacists. The average score on the pre-test knowledge indicator was 4.95 ± 0.39 and the average score on the post-test knowledge indicator was 7.81 ± 0.39. This was a significant improvement (p < 0.01). There was a significant increase in participant comfort level when counseling patients about sun safety after attending the CE program (p < 0.01). Personal experience with skin cancer did not have a significant effect on the pre-test knowledge indicator scores, however it was associated with the knowledge indicator change score (p < 0.01). Completion of previous skin cancer CE programs did not have a significant effect on the pre-test knowledge indicator score or the change score. Conclusions: Pharmacists who attended the CE program improved their knowledge indicator scores when tested about malignant melanoma and sun safety. Many participants felt more comfortable counseling patients about sun safety and felt their counseling on sun safety would change as a result of attending this CE program.

Malignant Melanoma

Continuing Education Program

Pharmacists

A Translational Study Evaluating the Uses of Diagnostic and Therapeutic Practices Established in Human Malignant Melanoma in Equine Malignant Melanoma

Moore, Jenna Sheree

31 May 2013

Malignant melanoma is a neoplasm of melanocytes. It typically originates in skin, but may metastasize to other body systems. It is a relatively common neoplasm in both humans and horses, with striking similarities across both species. Heritable genetic factors associated with melanoma have been identified in both human malignant melanoma (HMM) and equine malignant melanoma (EMM). This work investigates similarities and differences of EMM and HMM through comparative protein expression using immunohistochemical staining. Nestin, Pax-3/7, B-Raf, and SOX-10 are commonly expressed in HMM tissues. Expression of these proteins is not noted in normal human melanocytes, is associated with decreased melanocytic differentiation, and with increased proliferation leading to tumorigenesis. My findings demonstrate similar expression of these proteins in EMM. Aberrant protein expression patterns may signal underlying genetic mutations. Similar abnormal expression patterns suggest that EMM and HMM may share common genetic abnormalities. Treatment of malignant melanoma presents similar challenges in both horses and humans. In general, early stages of the disease can be successfully treated with surgical excision; however, advanced stages of EMM and HMM are often refractory. Therefore, development of novel therapies for advanced stages of melanoma is essential in both species, with the horse representing a useful model for this process. One novel therapy, frankincense oil (FO) is a resin distillate from trees of the genus Boswellia. Studies have demonstrated cytostatic and apoptotic-modulating properties of FO in various human cancer cell lines. No studies have evaluated FO as a therapy for skin neoplasms. In my work, the apoptotic properties of FO from Boswellia frereana were verified in a HMM cell line (SK-Mel-5). The cytotoxicity and therapeutic efficacy of FO were also studied by evaluating the effects of FO in cases of perianal EMM. FO was found to be consistently cytotoxic when injected directly into EMM tumors, but largely inconsequential when applied topically. FO was found to substantially decrease the size of injected masses. These findings suggest that FO could be useful for debulking large masses in late stage dermal EMM. The combined results of these studies support further investigation of EMM as a translational model for HMM. / Ph. D.

Equine melanoma

Malignant Melanoma

Frankincense oil

Boswellia

A study of matrix metalloproteinases in cancer and atherosclerosis

Laxton, Ross Campbell

January 2012

Background: Matrix metalloproteinases (MMPs) have been shown to be involved in cancers and atherosclerosis, the leading causes of present day mortality. The objectives of the cancer element of this project were to investigate single nucleotide polymorphisms (SNPs) in MMP1 and MMP8 regarding breast cancer and malignant melanoma, and a functional characterisation of the genetic variants, including the MMP1 polymorphism rs19799750, previously associated with multiple cancers. The objective of the second part of this project was to investigate whether MMP8 played a role in the development of atherosclerotic lesions and if so, the underlying mechanisms. Methods/Results: Genetic investigations found the MMP8 SNP rs11225395 to be associated with the occurrence of both breast cancer and malignant melanoma; furthermore it was also associated with reduced lymph node metastasis, reduced cancer relapse and greater survival. Functional luciferase assays showed that the minor allele of the polymorphism has higher promoter activity in breast cancer and melanoma cell lines. They also showed haplotypic effects on MMP1 promoter activity in several cancer cell lines by the 2G allele of polymorphism rs1799750 and one or more MMP1 promoter SNPS. The second part of the study found an association between a MMP8 SNP and the extent of coronary atherosclerosis; additionally a relationship among MMP8 gene variation, plasma VCAM-1 level, and atherosclerosis progression was observed in a prospective study. Murine studies showed reduced atherosclerosis in MMP8/ApoE knockout mice compared with ApoE knockout littermate controls. Biochemical studies confirmed that MMP8 can convert angiotensin I to angiotensin II. Conclusions: The data of the first part of this project support the notion that genetic polymorphisms in the MMP1 and MMP8 influence the expression of these genes and the development and progression of cancer. The results of the second part of this project indicate an important role of MMP8 in the pathogenesis of atherosclerosis.

616

Microdialysis as a Tool in Studies of L-Dopa and Metabolites in Malignant Melanoma and Parkinson’s Disease

Dizdar (Segrell), Nil

January 1999

A model with human melanoma xenografts transplanted to athymic mice has been adopted for in vivo studies of 5-S-cysteinyldopa (an intermediate pigment metabolite), glutathione, and cysteine. L-Dopa is an intermediate metabolite in pigment formation and is also important in the treatment of Parkinson's disease, and therefore 1 have also studied the pharmacokinetics of this compound. We were first to describe in vivo microdialysis in melanoma tissue and showed that dialysis membranes of cuprophane or polyamide are suitable for studies of interstitial 5-S-cysteinyldopa and selected thiols. Analytical procedures were also improved for quantitation of 5-S-cysteinyldopa, L-dopa, glutathione, cysteine, and N-acetylcysteine (NAC). In the melanoma xenografts the interstitial concentration of 5-S-cysteinyldopa reflected the high intracellular production of this intermediate metabolite. For in vivo manipulation of glutathione in the melanoma tissue we gave intraperitoneal injection of buthionine sulphoximine to the animals and thus reduced the glutathione concentrations substantially. We showed that restitution of glutathione in melanoma tissue occurs spontaneously and is not much improved by treatment with the cysteine deliverers NAC and L-2-oxothiazolidine-4-carboxylate (OTC). 5-S-Cysteinyldopa was not substantially affected by great variations in glutathione concentrations. Transport of NAC from intraperitoneal injection to melanoma tissue occurred rapidly and deacetylation to cysteine in vivo could be detected soon after NAC injection. In vivo formation of cysteine was slower from OTC than from NAC. Pharmacokinetic studies of L-dopa in human subjects indicated a slight to moderate protein binding. Plasma free L-dopa had similar elimination T½ as interstitial L-dopa, but in some cases the elimination of total L-dopa was slower. Difficulties in intestinal absorption of L-dopa were revealed by microdialysis in blood and subcutaneous tissue. Studies showed that this was due to delayed emptying of the stomach. L-Dopa intake increased 5-S-cysteinyldopa concentrations in blood within 30 min in patients with Parkinson's disease and a history of melanoma. No melanoma activation occurred during long-term treatment with L-dopa. Microdialysis is thus a safe and easily applied method for in vivo studies of both pigment metabolites from human melanoma tissue transplanted to nude mice and for pharmacokinetic studies of L-dopa. / On the day of the public defence the status of the articles IV, V and VI was: Submitted.

Microdialysis

L-Dopa

Malignant Melanoma

Parkinson's Disease

in vivo

MEDICINE

MEDICIN

Perfil de expressão do receptor do peptídeo liberador de gastrina em materiais de biópsia de pacientes portadores de melanoma maligno

Marrone, Bianca Fontana

January 2012

Introdução: A incidência de melanoma maligno (MM) está aumentando mundialmente e o manejo de pacientes com doença avançada representa um difícil problema. Durante décadas, a quimioterapia foi o tratamento padrão no tratamento de pacientes com MM metastático. Entretanto, essa modalidade tem produzido resultados desapontadores. Recentemente, com os avanços no conhecimento sobre os eventos moleculares relacionados ao desenvolvimento do MM, novas drogas dirigidas a alvos moleculares de relevância na doença têm sido identificadas. O peptídeo liberador de gastrina (GRP) é um peptídeo neuroendócrino, o qual possui efeito estimulador no crescimento em vários tipos de neoplasias murinas e humanas. Poucos dados são conhecidos em relação à expressão de receptores de GRP (GRPR) em materiais de biópsia de pacientes portadores de MM. A identificação de uma expressão elevada destes receptores no MM poderá permitir uma maior compreensão sobre a biologia desta neoplasia, bem como embasar estudos com o uso de moduladores desta via de sinalização com potencial ação terapêutica. Objetivos: O objetivo desse estudo foi determinar a expressão de receptores de GRP em biópsias de pacientes com MM, bem como buscar eventuais correlações entre os níveis de expressão de GRPR e fatores prognósticos reconhecidos nesta doença. Métodos: Foi realizado um estudo imuno-histoquímico (IHQ) em blocos fixados em formalina e embebidos em parafina, contendo material de biópsia de 51 pacientes portadores de MM cutâneo. Utilizou-se um anticorpo policlonal de coelho anti-GRPR (OPA1-15619, Affinity Bioreagents, USA). Após a quantificação da expressão de GRPR nas amostras, foram analisadas as diferenças de expressão entre subgrupos prognósticos, com a aplicação do teste exato de Fisher. Resultados: A expressão de GRPR foi demonstrada no citoplasma de 42 das 51 (82,4%) amostras de MM cutâneo. A expressão foi considerada forte em 30 amostras (58,9%). Não foi observada diferença significativa na expressão de GRPR quando foram analisadas amostras de MM em sítio primário versus metastático. Foram correlacionados os escores da expressão de GRPR com os achados patológicos associados ao prognóstico do MM cutâneo primário, não tendo sido detectadas diferenças significativas com relação aos níveis de Clark (p=0,35) e Índice espessura de Breslow (p= 0,175). Conclusão: Nosso trabalho mostrou uma expressão de GRPR em amostras de MM cutâneo na vasta maioria dos casos (82,4%). Em 30 amostras (58.3%), a expressão de GRPR foi considerada de forte intensidade. Não houve associação entre a intensidade de expressão de GRPR quando comparadas amostras de sítio primário versus metastático, níveis de Clark ou índices de Breslow. Este estudo é um dos primeiros na literatura a descrever uma expressão de GRPR elevada em amostras obtidas de pacientes portadores de MM cutâneo. Estudos subsequentes, preferencialmente com um maior número amostral, são necessários para confirmar estes achados e permitir melhor análise da expressão deste receptor em distintos subgrupos prognósticos. Se confirmados, os nossos dados podem justificar a realização de estudos que explorem novas estratégias terapêuticas utilizando agentes moduladores da expressão de GRPR em pacientes com MM refratário ao tratamento convencional. / Background: The incidence of malignant melanoma (MM) is increasing worldwide and the management of patients with disseminated disease is a difficult problem. Chemotherapy was the treatment of choice in metastatic melanomas for many decades. However, this option produces disappointing results. Recently, the better understanding about molecular events related do the development of MM allowed the development of new drugs directed against specific molecular targets. The gastrin-releasing peptide (GRP) is a neuroendocrine peptide shown to have growth-stimulatory effects on many types of murine and human cancers. Few data are available about GRP receptor (GRPR) expression in MM. The understanding about the molecular biology of MM may allow the identification of novel intracellular pathways of relevance in this disease, and potential GRPR modulators of therapeutic application in patients with refractory MM. Objectives: The aim of this study was to determine the GRPR expression in biopsy samples of patients with cutaneous MM, as well as to correlate its expression with known prognostic factors of relevance in this disease. Methods: Immunohistochemistry was performed on formalin-fixed, paraffin-embedded biopsy samples from 51 patients with cutaneous MM. A rabbit polyclonal anti-GRPR antibody (OPA1-15619, Affinity Bioreagents, USA) was used. Following the quantification of GRPR expression in the samples, the differences in GRPR expression among distinct prognostic MM subgroups were analyzed, using the Fisher´s test. Results: GRPR immunoexpression was demonstrated in cytoplasm of 42/51 (82.4%) cutaneous MM cases. It was strongly expressed in 30 (58.9%) of the samples. No significant differences between GRPR expression neither in relation to the primary or metastatic site, nor among known prognostic subgroups Clark´s level (p=0.35) and Breslow index ( p= 0.175) was observed. Conclusion: Our study has demonstrated the occurrence of a high GRPR expression in tumor specimens obtained from patients with cutaneous MM (82,4%). In 30 samples, a strong intensity of expression was documented (58.3%). No correlation was observed between the level of GRPR expression in primary or metastatic sites, nor for distinct Clark´s levels or Breslow index. This is one of the first studies demonstrating a high GRPR expression in tumor samples from patients with MM. Further studies are warranted, preferably including a larger patient population, to allow a better analysis of the expression of these receptors in different prognostic subgroups. If these observations are confirmed, the therapeutic use of GRPR inhibitors should be considered in patients with advanced MM who failed conventional treatments.

Melanoma

Peptídeo liberador de gastrina

Gastrin-releasing peptide

Malignant melanoma

Bombesin

Perfil de expressão do receptor do peptídeo liberador de gastrina em materiais de biópsia de pacientes portadores de melanoma maligno

Marrone, Bianca Fontana

January 2012

Introdução: A incidência de melanoma maligno (MM) está aumentando mundialmente e o manejo de pacientes com doença avançada representa um difícil problema. Durante décadas, a quimioterapia foi o tratamento padrão no tratamento de pacientes com MM metastático. Entretanto, essa modalidade tem produzido resultados desapontadores. Recentemente, com os avanços no conhecimento sobre os eventos moleculares relacionados ao desenvolvimento do MM, novas drogas dirigidas a alvos moleculares de relevância na doença têm sido identificadas. O peptídeo liberador de gastrina (GRP) é um peptídeo neuroendócrino, o qual possui efeito estimulador no crescimento em vários tipos de neoplasias murinas e humanas. Poucos dados são conhecidos em relação à expressão de receptores de GRP (GRPR) em materiais de biópsia de pacientes portadores de MM. A identificação de uma expressão elevada destes receptores no MM poderá permitir uma maior compreensão sobre a biologia desta neoplasia, bem como embasar estudos com o uso de moduladores desta via de sinalização com potencial ação terapêutica. Objetivos: O objetivo desse estudo foi determinar a expressão de receptores de GRP em biópsias de pacientes com MM, bem como buscar eventuais correlações entre os níveis de expressão de GRPR e fatores prognósticos reconhecidos nesta doença. Métodos: Foi realizado um estudo imuno-histoquímico (IHQ) em blocos fixados em formalina e embebidos em parafina, contendo material de biópsia de 51 pacientes portadores de MM cutâneo. Utilizou-se um anticorpo policlonal de coelho anti-GRPR (OPA1-15619, Affinity Bioreagents, USA). Após a quantificação da expressão de GRPR nas amostras, foram analisadas as diferenças de expressão entre subgrupos prognósticos, com a aplicação do teste exato de Fisher. Resultados: A expressão de GRPR foi demonstrada no citoplasma de 42 das 51 (82,4%) amostras de MM cutâneo. A expressão foi considerada forte em 30 amostras (58,9%). Não foi observada diferença significativa na expressão de GRPR quando foram analisadas amostras de MM em sítio primário versus metastático. Foram correlacionados os escores da expressão de GRPR com os achados patológicos associados ao prognóstico do MM cutâneo primário, não tendo sido detectadas diferenças significativas com relação aos níveis de Clark (p=0,35) e Índice espessura de Breslow (p= 0,175). Conclusão: Nosso trabalho mostrou uma expressão de GRPR em amostras de MM cutâneo na vasta maioria dos casos (82,4%). Em 30 amostras (58.3%), a expressão de GRPR foi considerada de forte intensidade. Não houve associação entre a intensidade de expressão de GRPR quando comparadas amostras de sítio primário versus metastático, níveis de Clark ou índices de Breslow. Este estudo é um dos primeiros na literatura a descrever uma expressão de GRPR elevada em amostras obtidas de pacientes portadores de MM cutâneo. Estudos subsequentes, preferencialmente com um maior número amostral, são necessários para confirmar estes achados e permitir melhor análise da expressão deste receptor em distintos subgrupos prognósticos. Se confirmados, os nossos dados podem justificar a realização de estudos que explorem novas estratégias terapêuticas utilizando agentes moduladores da expressão de GRPR em pacientes com MM refratário ao tratamento convencional. / Background: The incidence of malignant melanoma (MM) is increasing worldwide and the management of patients with disseminated disease is a difficult problem. Chemotherapy was the treatment of choice in metastatic melanomas for many decades. However, this option produces disappointing results. Recently, the better understanding about molecular events related do the development of MM allowed the development of new drugs directed against specific molecular targets. The gastrin-releasing peptide (GRP) is a neuroendocrine peptide shown to have growth-stimulatory effects on many types of murine and human cancers. Few data are available about GRP receptor (GRPR) expression in MM. The understanding about the molecular biology of MM may allow the identification of novel intracellular pathways of relevance in this disease, and potential GRPR modulators of therapeutic application in patients with refractory MM. Objectives: The aim of this study was to determine the GRPR expression in biopsy samples of patients with cutaneous MM, as well as to correlate its expression with known prognostic factors of relevance in this disease. Methods: Immunohistochemistry was performed on formalin-fixed, paraffin-embedded biopsy samples from 51 patients with cutaneous MM. A rabbit polyclonal anti-GRPR antibody (OPA1-15619, Affinity Bioreagents, USA) was used. Following the quantification of GRPR expression in the samples, the differences in GRPR expression among distinct prognostic MM subgroups were analyzed, using the Fisher´s test. Results: GRPR immunoexpression was demonstrated in cytoplasm of 42/51 (82.4%) cutaneous MM cases. It was strongly expressed in 30 (58.9%) of the samples. No significant differences between GRPR expression neither in relation to the primary or metastatic site, nor among known prognostic subgroups Clark´s level (p=0.35) and Breslow index ( p= 0.175) was observed. Conclusion: Our study has demonstrated the occurrence of a high GRPR expression in tumor specimens obtained from patients with cutaneous MM (82,4%). In 30 samples, a strong intensity of expression was documented (58.3%). No correlation was observed between the level of GRPR expression in primary or metastatic sites, nor for distinct Clark´s levels or Breslow index. This is one of the first studies demonstrating a high GRPR expression in tumor samples from patients with MM. Further studies are warranted, preferably including a larger patient population, to allow a better analysis of the expression of these receptors in different prognostic subgroups. If these observations are confirmed, the therapeutic use of GRPR inhibitors should be considered in patients with advanced MM who failed conventional treatments.

Melanoma

Peptídeo liberador de gastrina

Gastrin-releasing peptide

Malignant melanoma

Bombesin

Perfil de expressão do receptor do peptídeo liberador de gastrina em materiais de biópsia de pacientes portadores de melanoma maligno

Marrone, Bianca Fontana

January 2012

Introdução: A incidência de melanoma maligno (MM) está aumentando mundialmente e o manejo de pacientes com doença avançada representa um difícil problema. Durante décadas, a quimioterapia foi o tratamento padrão no tratamento de pacientes com MM metastático. Entretanto, essa modalidade tem produzido resultados desapontadores. Recentemente, com os avanços no conhecimento sobre os eventos moleculares relacionados ao desenvolvimento do MM, novas drogas dirigidas a alvos moleculares de relevância na doença têm sido identificadas. O peptídeo liberador de gastrina (GRP) é um peptídeo neuroendócrino, o qual possui efeito estimulador no crescimento em vários tipos de neoplasias murinas e humanas. Poucos dados são conhecidos em relação à expressão de receptores de GRP (GRPR) em materiais de biópsia de pacientes portadores de MM. A identificação de uma expressão elevada destes receptores no MM poderá permitir uma maior compreensão sobre a biologia desta neoplasia, bem como embasar estudos com o uso de moduladores desta via de sinalização com potencial ação terapêutica. Objetivos: O objetivo desse estudo foi determinar a expressão de receptores de GRP em biópsias de pacientes com MM, bem como buscar eventuais correlações entre os níveis de expressão de GRPR e fatores prognósticos reconhecidos nesta doença. Métodos: Foi realizado um estudo imuno-histoquímico (IHQ) em blocos fixados em formalina e embebidos em parafina, contendo material de biópsia de 51 pacientes portadores de MM cutâneo. Utilizou-se um anticorpo policlonal de coelho anti-GRPR (OPA1-15619, Affinity Bioreagents, USA). Após a quantificação da expressão de GRPR nas amostras, foram analisadas as diferenças de expressão entre subgrupos prognósticos, com a aplicação do teste exato de Fisher. Resultados: A expressão de GRPR foi demonstrada no citoplasma de 42 das 51 (82,4%) amostras de MM cutâneo. A expressão foi considerada forte em 30 amostras (58,9%). Não foi observada diferença significativa na expressão de GRPR quando foram analisadas amostras de MM em sítio primário versus metastático. Foram correlacionados os escores da expressão de GRPR com os achados patológicos associados ao prognóstico do MM cutâneo primário, não tendo sido detectadas diferenças significativas com relação aos níveis de Clark (p=0,35) e Índice espessura de Breslow (p= 0,175). Conclusão: Nosso trabalho mostrou uma expressão de GRPR em amostras de MM cutâneo na vasta maioria dos casos (82,4%). Em 30 amostras (58.3%), a expressão de GRPR foi considerada de forte intensidade. Não houve associação entre a intensidade de expressão de GRPR quando comparadas amostras de sítio primário versus metastático, níveis de Clark ou índices de Breslow. Este estudo é um dos primeiros na literatura a descrever uma expressão de GRPR elevada em amostras obtidas de pacientes portadores de MM cutâneo. Estudos subsequentes, preferencialmente com um maior número amostral, são necessários para confirmar estes achados e permitir melhor análise da expressão deste receptor em distintos subgrupos prognósticos. Se confirmados, os nossos dados podem justificar a realização de estudos que explorem novas estratégias terapêuticas utilizando agentes moduladores da expressão de GRPR em pacientes com MM refratário ao tratamento convencional. / Background: The incidence of malignant melanoma (MM) is increasing worldwide and the management of patients with disseminated disease is a difficult problem. Chemotherapy was the treatment of choice in metastatic melanomas for many decades. However, this option produces disappointing results. Recently, the better understanding about molecular events related do the development of MM allowed the development of new drugs directed against specific molecular targets. The gastrin-releasing peptide (GRP) is a neuroendocrine peptide shown to have growth-stimulatory effects on many types of murine and human cancers. Few data are available about GRP receptor (GRPR) expression in MM. The understanding about the molecular biology of MM may allow the identification of novel intracellular pathways of relevance in this disease, and potential GRPR modulators of therapeutic application in patients with refractory MM. Objectives: The aim of this study was to determine the GRPR expression in biopsy samples of patients with cutaneous MM, as well as to correlate its expression with known prognostic factors of relevance in this disease. Methods: Immunohistochemistry was performed on formalin-fixed, paraffin-embedded biopsy samples from 51 patients with cutaneous MM. A rabbit polyclonal anti-GRPR antibody (OPA1-15619, Affinity Bioreagents, USA) was used. Following the quantification of GRPR expression in the samples, the differences in GRPR expression among distinct prognostic MM subgroups were analyzed, using the Fisher´s test. Results: GRPR immunoexpression was demonstrated in cytoplasm of 42/51 (82.4%) cutaneous MM cases. It was strongly expressed in 30 (58.9%) of the samples. No significant differences between GRPR expression neither in relation to the primary or metastatic site, nor among known prognostic subgroups Clark´s level (p=0.35) and Breslow index ( p= 0.175) was observed. Conclusion: Our study has demonstrated the occurrence of a high GRPR expression in tumor specimens obtained from patients with cutaneous MM (82,4%). In 30 samples, a strong intensity of expression was documented (58.3%). No correlation was observed between the level of GRPR expression in primary or metastatic sites, nor for distinct Clark´s levels or Breslow index. This is one of the first studies demonstrating a high GRPR expression in tumor samples from patients with MM. Further studies are warranted, preferably including a larger patient population, to allow a better analysis of the expression of these receptors in different prognostic subgroups. If these observations are confirmed, the therapeutic use of GRPR inhibitors should be considered in patients with advanced MM who failed conventional treatments.

Melanoma

Peptídeo liberador de gastrina

Gastrin-releasing peptide

Malignant melanoma

Bombesin