Thèses sur le sujet « Epidermal Growth Factor Breast Neoplasms Breast Neoplasms »

Thesis (Ph. D.)--West Virginia University, 2004.
Title from document title page. Document formatted into pages; contains x, 160 p. : ill. (some col.). Vita. Includes abstract. Includes bibliographical references.

Uvod: Karcinom dojke je heterogena bolest koju karakterišu različita morfologija, imunohisto-hemijski profil, klinički tok i terapijski odgovor. Ki-67 proliferativni indeks je jedan od markera sa prognostičkim i prediktivnim značajem, čije metodološko određivanje i analiza još uvek nisu standardizovani. Cilj: Utvrditi graničnu (“cut-off”) prognostičku vrednost Ki-67 indeksa, kao i povezanost vrednosti Ki-67 u ranom luminalnom karcinomu dojke sa prognostičkim i prediktivnim parametrima karcinoma dojke, kao što su životna dob bolesnica, veličina tumora, histološki gradus (HG) i nivo tumorske ekspresije receptora estrogena (ER) i progesterona (PR). Takođe, cilj istraživanja je i utvrđivanje značajnosti razlike u vrednosti Ki-67 proliferativnog indeksa u odnosu na pojavu lokalnog recidiva, udaljenih metastaza i dužinu preživljavanja u toku petogodišnjeg perioda praćenja pacijentkinja. Metode: Retrospektivno je analizirano 120 patohistoloških izveštaja bolesnica kojima je u periodu od 01.01.2009. godine do 31.12.2011. godine na Institutu za onkologiju Vojvodine imunohistohemijskom analizom dokazan luminalni karcinom dojke (pozitivan ER i PR, negativan HER2), bez metastaza u aksilarnim limfnim čvorovima. Rezultati: Metodama deskriptivne statistike prosečna starost pacijentkinja je iznosila 57,42±10,17 godina; prosečna veličina tumora 17,98±6,97mm; recidiv je registrovan kod 8 (6,7%) pacijentkinja uz prosečan vremenski period do pojave recidiva od 49±20,23 meseci. Vrednost “cut off” indeksa Ki-67 od prognostičkog značaja za vremenski period bez recidiva je iznosio 20,75%. Nije dokazana signifikantna veza između vrednosti Ki-67 i godina starosti pacijentkinja (p=0,401, odnosno p=0,293), kao i jačine ekspresije ER (p=1,00, p=0,957) i PR (p=0,273, p=0,189). Ustanovljena je signifikantna povezanost Ki-67 postoji sa veličinom (p=0,035, p=0,20) i HG tumora (p=0,041, p=0,20). Prosečan period praćenja bolesnica iznosio je 72,92±8,38 meseci; nije registrovana pojava udaljenih metastaza, kao ni smrtni ishod. U odnosu na pojavu lokalnog recidiva, Kaplan-Majerovom analizom i Koksovom regresionom analizom proliferativni indeks Ki-67 se pokazao kao signifikantan prediktor za procenu ponovnog javljanja bolesti, lokalnog recidiva (Log rank (df = 1) = 2,73; p=0,045). Takođe je ustanovljeno da je statistički značajan prediktor za procenu recidiva bolesti i starosna dob bolesnica (Log rank (df = 1) = 6,885; p=0,009). Intenzitet pozitivnosti ER i PR, veličina tumora i histološki gradus se nisu pokazali kao prediktori za pojavu recidiva luminalnih karcinoma dojke (p > 0,05). Zaključak: Zbog heterogene prirode oboljenja, korišćenjem standardnih histopatoloških faktora i biomarkera teško je predvideti tok i ishod karcinoma dojke. Ki-67 je proliferativni marker, čija visoka vrednost korelira sa faktorima loše prognoze.
Introduction: Breast cancer is a heterogeneous disease characterized by different morphology, immunohistochemical profile, clinical course and response to applied therapy. Ki-67 proliferative index is one of the prognostic and predictive factors, whose methodological determination and analysis are still unstandardized. Objective: Determination of cut-off value for Ki-67 index, its corelation in luminal breast carcinoma with patient's age, tumor size, histological grade (HG) and expression of estrogen (ER) and progesterone (PR). Also, the aim of the study was to determine the significance of the difference in the value of the Ki-67 proliferative index in relation to the occurrence of local relapse, distant metastases and survival rates during the five-year follow-up period of the patient. Methods: Retrospectively, we analysed 120 pathohistological reports of patients who were treated in the period from 01.01.2009 until 31.12.2011 at the Oncology Institute of Vojvodina, and to whom immunohistochemically was proven luminal breast cancer (positive ER and PR, negative HER2), without axillary lymph node metastases. Results: The average patient’s age was 57.42±10.17 years; average tumor size 17.98±6.97mm; recurrence was registered in 8 (6.7%) patients with average recurrence time of 49±20.23 months. "Cut off" Ki-67 value of prognostic significance for period without recurrence was 20.75%. Test didn’t show significant relationship between Ki-67 and patient’s age (p=0.401 and p=0.293), as well as the strength of expression ER (p=1.00, p=0.957) and PR (p=0.273, p=0.189). Significant correlation was present for Ki-67 with size (p=0.035, p=0.20) and tumor’s HG (p=0.041, p=0.20). The average follow-up period for patients was 72.92±8.38 months; there was no registered occurrence of distant metastases or fatal outcome. In relation to the occurrence of local relapse, Kaplan-Meier analysis and Cox regression analysis, the proliferative index Ki-67 proved to be a significant predictor for the assessment of recurrence of the disease, local relapse (Log rank (df = 1) = 2.73; p = 0.045). Also, it was founded that a statistically significant predictor for assessing the recurrence of the disease is the age of the patients (Log rank (df = 1) = 6.885; p = 0.009). The intensity of ER and PR expression, tumor size and histological grade have not been shown to be predictors of the recurrence of luminal breast carcinoma (p> 0.05). Conclusion: Breast carcinoma is heterogeneous disease, so it is difficult to predict its course and outcome using standard histopathological factors and biomarkers. Ki-67 is proliferative marker whose high value correlates with factors of bad prognosis.

INTRODUÇÃO: Os carcinomas HER-2 positivos representam cerca de 20- 30% de todos os tumores da mama e se caracterizam por curso clínico mais agressivo, com alta proliferação celular e resistência a apoptose, determinados por cascatas de sinalizações intracelulares, tais como a via PI3K/AKT. O trastuzumabe, um anticorpo monoclonal humanizado que se liga à molécula de HER-2, é o tratamento padrão destas pacientes. A resposta a monoterapia com trastuzumabe varia de 12-30% e a persistência da ativação da via PI3K/AKT é um dos mecanismos de resistência. A ativação do AKT começa com a fosforilação do PIP2 a PIP3 pela PI3K. A desfosforilação do PIP3 é mediada pela PTEN e sua deficiência é um dos fatores possivelmente implicados na resistência ao trastuzumabe. Além da resistência à terapêutica, os tumores HER-2 positivos são heterogêneos quanto ao seu comportamento biológico. A busca de diferentes padrões morfológicos e moleculares neste grupo de carcinomas pretende identificar subgrupos prognósticos e preditivos, permitindo a individualização terapêutica. OBJETIVOS: Estudar a expressão imunoistoquímica de duas moléculas da via de sinalização PI3K/AKT (PTEN e AKT fosforilada) e explorar a via de sinalização androgênica através da expressão do receptor de androgênio e dos perfis morfológico e molecular apócrinos. METODOLOGIA: O estudo foi retrospectivo com revisão dos preparados histológicos e construção de blocos de microarranjos com amostras dos tumores para estudo imunoistoquímico. Na revisão foram avaliados: tipo histológico, características morfológicas apócrinas, presença de componente in situ, graus histológico e nuclear, receptores de estrogênio e progesterona, e atividade proliferativa através da expressão imunoistoquímica do Ki-67. Os preparados histológicos foram submetidos à pesquisa de PTEN, AKT fosforilada e receptor de androgênio. Pacientes, familiares e médicos foram contatados para recuperação do seguimento e evolução. RESULTADOS: Foram estudadas 104 pacientes portadoras de carcinoma primário da mama. A expressão de PTEN esteve reduzida em 20/104 (19,2%) dos casos e foi mais freqüente nos tumores com AKT positivo (p= 0,06). O grupo de tumores sem perda de expressão de PTEN apresentou maior atividade proliferativa. A AKT foi positiva em 71/104 (68,3%) casos e se associou a maior grau de diferenciação e à expressão de receptor de androgênio. O receptor de androgênio foi positivo em 89/104 (85,6%) dos casos e esteve associado ao menor grau histológico (p=0,018), receptor de estrogênio (p=0,008) e menor atividade proliferativa (p=0,001). A ausência da expressão do receptor de estrogênio (perfil molecular apócrino) foi identificada em 41/104 casos (39,4%) e se associou a tumores com grau histológico mais alto. O perfil morfológico apócrino foi identificado em 71 (68,3%) dos casos e se associou a alto grau histológico e nuclear. O seguimento foi possível em 55 casos e observamos tendência a menor sobrevida livre de doença nos tumores AKTpositivos e RA-negativos. CONCLUSÕES: Nossos resultados comprovam a heterogeneidade dos carcinomas mamários HER-2 positivos e indicam diferenças em pelos menos duas vias de sinalização celulares como possíveis explicações para as mesmas: a via PI3K/AKT e a androgênica
BACKGROUND: HER-2 positive carcinomas represent about 20-30% of all breast tumors and are characterized by a more aggressive clinical course with high cell proliferation and apoptosis resistance, determined by cascades of intracellular signals, such as the PI3K/AKT pathway. Trastuzumab, a humanized monoclonal antibody that binds to HER-2 molecule, is the standard treatment for these patients. The response to monotherapy with trastuzumab ranges from 12-30% and the persistence of activation of the PI3K/AKT pathway is one of mechanisms of resistance. Activation of AKT begins with the phosphorylation of PIP2 to PIP3 by PI3K. The dephosphorylation of PIP3 is mediated by PTEN and its deficiency is one of the factors possibly involved in resistance to trastuzumab. In addition to resistance to therapy, HER-2 positive tumors are heterogeneous in their biologic behavior. The search for different morphological and molecular patterns of carcinomas in this group aims to identify prognostic and predictive subgroups, allowing for customized therapy. OBJECTIVES: To study the immunohistochemical expression of two molecules of the signaling pathway PI3K/AKT (phosphorylated AKT and PTEN) and to explore the androgen signaling pathway through the expression of androgen receptor and apocrine morphological and molecular profiles. METHODS: This study retrospectively reviewed the histological preparations and built tissue microarray with tumor samples for immunohistochemical study. We assessed histologic type, apocrine morphology, presence of in situ component, histologic and nuclear grade, estrogen and progesterone receptors and proliferative activity through the immunohistochemical expression of Ki-67. The tissue preparations were examined for PTEN, phosphorylated AKT and androgen receptor. Patients, relatives and physicians were contacted for retrieval of follow-up data. RESULTS: We studied 104 primary breast cancer patients. The expression of PTEN was reduced in 20/104 (19.2%) cases and was more frequent in tumors with positive AKT (p = 0.06). The group of tumors without loss of PTEN expression showed higher proliferative activity. AKT was positive in 71/104 (68.3%) cases and was associated with a higher degree of differentiation and with expression of androgen receptor. The androgen receptor was positive in 89/104 (85.6%) cases and was associated with lower histological grade (p = 0.018), estrogen receptor (p = 0.008) and lower proliferative activity (p = 0.001). The absence of expression of estrogen receptor (apocrine molecular profile) was identified in 41/104 cases (39.4%) and was associated with tumors of higher histologic grade. The apocrine morphological profile was identified in 71 (68.3%) cases and was associated with high histological grade and nuclear. Follow-up was possible in 55 cases and a trend for shorter disease-free survival was observed in AKT-positive and AR-negative tumors. CONCLUSIONS: Our results confirmed that HER-2-positive breast cancers are heterogeneous and indicate that differences in at least two cellular signaling pathways PI3K/AKT and androgen pathway might underliy such a heterogeneity

This thesis concerns a melanoma-derived growth regulatory factor that inhibited proliferation of several malignant human cell lines, and, in particular, a line designated UCT-BR-1, which was derived from a human breast cancer metastasis. The work is presented in four chapters. Chapter 1 provides a review of the relevant literature at the time of writing; Chapters 2 and 3 describe the experimental work that was done; and in Chapter 4 I discuss the implications of my results for current and future work in growth factors. Experimental results are presented as Charts (which may be Figures or Tables) and the methods and experimental protocols that I used are described in the Chart legends and not in the main text of the thesis. The Appendix contains details of the tissue culture techniques and descriptions of the cell lines that were used. Sources of the various laboratory materials as well as the methods that were employed for the more routine procedures are also described in the appendix.

Beclin 1 is a haplo-insufficient tumor suppressor that is decreased in many human tumors. The function of Beclin 1 in cancer has been attributed primarily to its role in the degradative process of autophagy. However, the role of autophagy itself in tumorigenesis is context-dependent and can be both preventive and promoting. Due to its dual function in cancer a better understanding of this process is necessary to develop potential novel cancer therapies. To gain insight into the role of autophagy in breast carcinoma, I analyzed the autophagydependency of different subtypes of breast cancer. My results implicate that triple-negative breast carcinoma cells are more dependent on autophagy than luminal breast carcinoma cells. Chemical inhibition of autophagy decreased the tumorigenicity of triple-negative breast carcinoma cells with regard to proliferation and anchorage-independent growth. However, RNAi-mediated suppression of two autophagy genes, ATG5 and Beclin 1, revealed different outcomes. While suppression of ATG5 decreased glycolysis, Beclin 1 depletion did not affect the glycolytic rates. These results suggest autophagy-independent pro-tumorigenic effects of loss of Beclin 1 in cancer. Beclin 1 is a core component of the Vps34/Class III PI3K (PI3KC3) and Vps15/p150 complex that regulates multiple membrane trafficking events. I describe a novel mechanism of action for Beclin 1 in breast cancer involving its control of growth factor receptor signaling. I identify a specific stage of early endosome maturation that is regulated by Beclin 1, the transition of APPL1- containing phosphatidyIinositol 3-phosphate-negative (PI3P-) endosomes to PI3P+ endosomes. Beclin 1 regulates PI3P production in response to growth factor stimulation to control the residency time of growth factor receptors in the PI3P-/APPL+ signaling competent compartment. As a result, suppression of BECN1 sustains growth factor stimulated AKT and ERK activation resulting in increased breast carcinoma cell invasion. In human breast tumors, Beclin 1 expression is inversely correlated with AKT and ERK phosphorylation. Taken together my data identify a novel role for Beclin 1 in regulating growth factor signaling and reveal a mechanism by which loss of Beclin 1 expression would enhance breast cancer progression independent of its impact on autophagy.

Orientador: Luis Otavio Zanatta Sarian
Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas
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Resumo: Introdução: A via de sinalização intracelular PTEN, mTOR, PI3K, IGF-1R e EGFR exerce papel prognóstico importante no câncer de mama. Embora muitos estudos tenham analisado a correlação entre as alterações gênicas de PTEN, mTOR, PI3K, IGF-1R e EGFR e o mau prognóstico em câncer de mama, há uma lacuna na literatura com relação ao valor prognóstico dessas proteínas na adjuvância do câncer de mama. Apesar de existirem fatores prognósticos e preditivos conhecidos, como os receptores hormonais e o HER-2, no campo imunológico, o câncer de mama é um dos tumores menos imunogênicos. As proteínas PD-L1 e PD-L2 fazem parte de uma importante resposta imune antitumoral. Em câncer de mama, o valor prognóstico de PD-L1 e PD-L2 ainda não está definido. Objetivos: Investigar a expressão das proteínas PTEN, mTOR, PI3K, IGF-1R e EGFR e das proteínas PD-L1 e PD-L2, e a correlação com as características clínicas e patológicas do câncer de mama, sobrevida livre de doença e sobrevida global. Métodos: Foi realizada uma coorte que avaliou 192 casos de câncer de mama, estadios I, II e III, tratadas entre 1994 e 2014 no Hospital da Mulher (CAISM) da UNICAMP. Os dados clínicos e de sobrevida foram retirados de prontuários. Blocos de parafina foram utilizados para construção do microarranjo de tecidos (TMA). No TMA foi utilizada a técnica de imunohistoquímica (IHQ) para estudo da expressão dessas proteínas. A terapia adjuvante foi administrada de acordo com o protocolo de tratamento institucional. Resultados: A expressão de PTEN foi encontrada em 40.6% (77/190); mTOR em 47.4% (90/190); PI3K em 29.8% (57/191); IGF-1R em 35.8% (68/190) e EGFR em 25.7% (49/191). Nas células do câncer de mama, a expressão de PTEN ocorreu no citoplasma e na região nuclear; a expressão de mTOR foi constatada de modo intenso na região nuclear e também no citoplasma. A expressão de PI3K foi mais intensa na membrana celular e menos intensa no citoplasma. A expressão de IGF-1R foi detectada na membrana celular das células tumorais. A expressão de todas essas proteínas foi significativamente associada à presença de linfonodos positivos. A idade mais jovem ao diagnóstico foi associada à expressão de PTEN e PI3K. A presença de tumores maiores foi associada à expressão de PTEN. Os receptores de progesterona negativos foram associados à expressão de PI3K. Receptores de estrógeno negativos e recorrência à distância foram ambos associados à expressão de EGFR. As expressões de PTEN, PI3K e EGFR foram fortemente associadas a características clínicas e patológicas de pior prognóstico. A expressão de PI3K foi significativamente associada à pior sobrevida livre de progressão (p=0.04) e pior sobrevida global (p=0.04). A expressão de EGFR foi também significativamente associada à pior sobrevida livre de progressão (p=0.03) e pior sobrevida global (p=0.04). A expressão de PTEN não foi associada à sobrevida. A expressão de PD-L1 foi identificada em 56.7% (107/189) e a de PD-L2 em 50.8% (97/192). Enquanto a expressão de PD-L1 foi detectada na membrana celular e no citoplasma das células do câncer de mama, a expressão de PD-L2 ocorreu no citoplasma e na região nuclear. Idade mais jovem ao diagnóstico, linfonodos positivos, receptor de estrógeno negativo e recorrência à distância foram associados tanto à expressão de PD-L1 quanto à de PD-L2. A presença de tumores maiores e de alto grau histológico foi associada à expressão de PD-L1. A expressão de PD-L1 foi significativamente associada à melhor sobrevida global (p=0.04). Conclusão: A expressão de PTEN, PI3K e EGFR pode representar um tipo de câncer de mama mais agressivo. A expressão de PI3K e EGFR pode ser considerada um marcador de mau prognóstico em câncer de mama. A expressão de PD-L1, apesar de ser associada a características clínicas e patológicas de pior evolução, pode ser considerada um marcador de bom prognóstico em câncer de mama
Abstract: Introduction: The PTEN, mTOR, PI3K, IGF-1R and EGFR signaling pathway plays an important role in prognosis of breast cancer. Although many studies have analyzed the correlation between PTEN, mTOR, PI3K, IGF-1R, and EGFR genes alterations with poor prognosis in breast cancer, there is still a gap in the literature concerning the prognostic value of these proteins in the adjuvant setting. Despite there were some well-known predictive and prognostic factors, such as hormone receptors and HER-2, in the immune field, breast cancer is one of the less immunogenic tumors. PD-L1 and PD-L2 constitute an important antitumor immune response. In breast cancer, the prognostic value of PD-L1 and PD-L2 is still to be defined. Objectives: This study investigates PTEN, mTOR, PI3K, IGF-1R and EGFR proteins expression and PD-L1 and PD-L2 proteins expression, and their correlation with clinicopathological features, disease-free survival and overall survival. Methods: In order to assess these proteins expression, we conducted an immunohistochemistry study using a tissue microarray encompassing 192 breast cancer cases, stage I, II and III, treated between 1994 and 2014 at the Women¿s Hospital (CAISM) from UNICAMP. All clinical and outcome data were retrieved from medical charts. Adjuvant therapy was administered according to the institution¿s treatment protocol. Results: PTEN expression was found in 40.6% (77/190); mTOR expression in 47.4% (90/190); PI3K expression in 29.8% (57/191); IGF-1R expression in 35.8% (68/190); and EGFR expression in 25.7% (49/191). In breast cancer cells PTEN expression showed cytoplasmic and nuclear immunoreactivity, and mTOR expression revealed strong nuclear and cytoplasmic staining. Tumors harboring PI3K expression presented strong immunoreactivity at cell membrane and weak cytoplasmic staining. IGF-1R expression was detected in breast cancer cell membrane. All proteins expression was significantly associated with lymph node positivity. Younger age at diagnosis was related to PTEN and PI3K expression. The presence of larger tumors was associated with PTEN expression. Negative progesterone receptor was correlated to PI3K expression. Estrogen receptor negativity and recurrence at distant sites were associated with EGFR expression. The expression of PTEN, PI3K, and EGFR were strongly associated with clinical and pathological features of poor prognosis. In our cohort, PI3K expression was associated with significantly worse disease-free survival (p=0.04) and overall survival (p=0.04), and EGFR expression was also significantly associated with worse disease-free survival (p=0.03) and overall survival (p=0.04). PD-L1 expression was present in 56.7% (107/189), and PD-L2 expression was identified in 50.8% (97/192). In breast cancer cells PD-L1 expression revealed strong immunoreactivity at cell membrane and cytoplasmic staining, and PD-L2 expression showed cytoplasmic and nuclear immunoreactivity. Younger age at diagnosis, lymph node positivity, estrogen negative receptor, and recurrence at distant sites were all associated with both PD-L1 and PD-L2 expression. The presence of larger tumors and higher histological grade were both associated with PD-L1 expression. PD-L1 expression was significantly associated with better overall survival (p=0.04) in breast cancer patients. Conclusion: The expression of PTEN, PI3K, and EGFR can represent a more aggressive type of breast cancer. PI3K and EGFR expressions emerge as poor prognostic markers in breast cancer. Despite its association with poor clinical and pathological features, PD-L1 expression seems to be a good prognostic marker in breast cancer
Doutorado
Oncologia Ginecológica e Mamária
Doutor em Ciências da Saúde

Thesis (Ph.D. in Pharmacology) -- University of Colorado Denver, 2007.
Typescript. Non-Latin script record Includes bibliographical references (leaves 112-128). Free to UCD affiliates. Online version available via ProQuest Digital Dissertations;

The 21st century brought about a dramatic increase in knowledge about genetic and molecular profiles of cancer. This information has validated the complexity of tumor cells and increased awareness of “nodal proteins”, but has yet to advance the development of rational targeted cancer therapeutics. Nodal proteins are critical cellular proteins that collect biological inputs and distribute the information across diverse biological processes. Survivin acts as a nodal protein by interfacing the multiple signals involved in mitosis and apoptosis and functionally integrate proliferation, cell death, and cellular homeostasis. By characterizing survivin as a target of both Type 1 Insulin-like Growth Factor (IGF-1) and Notch developmental signaling, we contribute to the paradigm of survivin as a nodal protein. The two signaling systems, Notch and IGF-1, regulate survivin by two independent mechanisms. Notch activation induces survivin transcription preferentially in basal breast cancer, a breast cancer subtype with poor prognosis and lack of molecular therapies. Activated Notch binds the transcription factor RBP-Jк and drives transcription from the survivin promoter. Notch mediated survivin expression increases cell cycle kinetics promoting tumor proliferation. Inhibition of Notch in a breast xenograft model reduced tumor growth and systemic metastasis. On the other hand, IGF-1 signaling drives survivin protein translation in prostate cancer cells. Binding of IGF-1 to its receptor activates downstream kinases, mammalian target of rapamycin (mTOR) and p70 S6 protein kinase (p70S6K), which modulates survivin mRNA translation to increase the apoptotic threshold. The multiple roles of survivin in tumorigenesis implicate survivin as a rational target for the “next generation” of cancer therapeutics.

A superexpressão de receptores HER-2 é anormalidade celular de grande relevância clínica no câncer de mama. Ela ocorre em aproximadamente 30% de carcinomas de mama incluindo lesões pré-neoplásicas e malignas, e está associada a prognóstico desfavorável. A hiperativação dos receptores HER-2, consequência natural de sua superexpressão, promove proliferação celular aberrante e tumorigênese. Admite-se que a ativação e envio de sinais via HER-2 possa acontecer quando estes receptores se encontram em compartimentos específicos da membrana celular, os lipid rafts. Assim, um número maior de HER-2 poderia implicar em maior quantidade de lipis rafts. Para testar essa hipótese, usamos modelo de transformação oncogênica que nos permitiu avaliar, especificamente, os efeitos da superexpressão de HER-2 e identificar a quantidade de lipid rafts. Para isso utilizamos a linhagem celular HB4a, derivada de célula epitelial luminal do tecido mamário humano normal com baixa expressão de HER-2; e a linhagem HB4aC5.2, um clone derivado da HB4a, que superexpressa receptores HER-2. Nas células HB4aC5.2, a superexpressão de HER-2 foi acompanhada pelo aumento dos lipid rafts na membrana celular, bem como, hiperativação de sinais de sobrevivência, proliferação (aumento da ativação de proteínas Akt e Erk1/2, respectivamente), e taxa de proliferação celular duas vezes mais rápida que a linhagem normal HB4a. Adicionalmente, a superexpressão de HER-2 foi associada com aumento da lipogênese celular (fenótipo lipogênico), dependente do aumento de ativação da enzima FASN e da superexpressão de DEPTOR. A FASN é responsável pela síntese de palmitato, utilizado para formação de lipid rafts. A superexpressão de DEPTOR, por modular a atividade transcricional de PPAR?, pode evitar a lipotoxicidade do excesso de palmitato. Além disso, DEPTOR, por sua capacidade em reduzir atividade do complexo mTORC1, contribui para sobrevivência celular dependente da proteína Akt. Em continuidade, consideramos, como segunda hipótese, que a desestruturação de lipid rafts poderia influenciar negativamente a ativação dos receptores HER-2. Para isso tratamos, as mesmas linhagens celulares anteriormente descritas, com ácido docosaexaenoico (DHA), um tipo de ácido graxo ômega-3. Nossos resultados mostraram que, nas células HB4aC5.2, o tratamento com DHA desestruturou os lipid rafts, inibiu a sinalização iniciada pelos receptores HER-2 ( diminuição da ativação das proteínas Akt, Erk1/2, FASN, atividade transcricional de PPAR? e expressão de DEPTOR) e reverteu o fenótipo lipogênico. Adiciona-se que essas modificações celulares e moleculares foram acompanhadas por indução significativa de morte e apoptose. As mesmas alterações não foram observadas nas células normais HB4a. Em conclusão, o presente estudo reforça a associação entre a presença de HER-2 e lipid rafts. Adicionalmente aponta que a desestruturação de lipid rafts por DHA reduz a sinalização de HER-2. Por fim, sugere que distúrbios em lipid rafts, induzidos por DHA, possam representar ferramenta útil no controle da sinalização aberrante deflagrada pelos receptores HER-2, e aponta potencial terapêutico na suplementação de DHA para quimioprevenção e tratamento do câncer de mama HER-2 positivo.
HER-2 receptor overexpression is a cellular abnormality of great clinical significance in breast cancer. It is described in approximately 30% of breast carcinomas, including preneoplasic and malignant lesions, and is associated with poor prognosis. Hyperactivation of HER-2 receptors, a natural consequence of its overexpression, promotes aberrant cell proliferation and tumorigenesis. For signal activation and transduction to occur, HER-2 must be localized in specific compartments in the cell membrane: the lipid rafts. Therefore, we hypothesize that a greater number of HER-2 receptors could indicate a greater quantity of lipid rafts. To test this, we used an oncogenic transformation model that specifically allowed assessment of the effects of HER-2 overexpression and identification of the quantity of lipid rafts: an HB4a cell line derived from normal human breast tissue luminal epithelial cells with low HER-2 expression, and an HB4aC5.2 cell line, a clone derived from HB4a that overexpresses HER-2 receptors. In the HB4aC5.2 cells, HER-2 overexpression was accompanied by an increase in lipid rafts in cell membranes as well as hyperactivation of survival signals, proliferation (increased activation of the proteins Akt and ERK1/2, respectively), and an increased rate of proliferation, compared to the normal HB4a line. In addition, HER-2 overexpression was associated with increased cellular lipogenesis (lipogenic phenotype), dependent on the increased activation of the FASN enzyme and the overexpression of DEPTOR. FASN is responsible for the synthesis of palmitate, used to synthesize lipid rafts. Overexpression of DEPTOR by modulating PPAR? transcriptional activity, may avoid lipotoxicity from excess palmitate. Moreover, DEPTOR, with its ability to reduce mTORC1 complex activity, contributes to cell survival dependent on Akt. To continue, we considered as a second hypothesis that the disruption of lipid rafts could negatively influence HER-2 receptor activation. For this, we treated the same cell lines described above with docosahexaenoic acid (DHA), a omega-3 fatty acid. Our results showed that in HB4aC5.2 cells DHA treatment disrupted the lipid rafts, inhibited signaling initiated by HER-2 receptors (reduced activation of Akt, ERK1/2, and FASN proteins, PPAR? transcriptional activity, and DEPTOR expression) and reversed the lipogenic phenotype. In addition, these cellular and molecular changes were accompanied by a significant induction of apoptosis and death. The same changes were not observed in normal HB4a cells. In conclusion, the present study reinforces the association between HER-2 presence and lipid rafts. It also indicates that the disruption of lipid rafts by DHA reduces HER-2 signaling. Finally, it suggests that DHA-induced disturbances in lipid rafts may represent a useful tool in controlling aberrant signaling triggered by HER-2 receptors, and indicate therapeutic potential in DHA supplementation for chemoprevention and treatment of HER-2 positive breast cancer.

Thesis (Ph.D. in Pharmacology) -- University of Colorado Denver, 2008.
Typescript. Includes bibliographical references (leaves 117-147). Free to UCD Anschutz Medical Campus. Online version available via ProQuest Digital Dissertations;

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Introduction: Hypoxia is a known adverse factor to cancer treatment, able to activate the signaling pathways PI3K and AMPK/Akt/mTOR, the two major pathways involved in the angiogenesis process. This process is regulated by many factors, being the most important factors the Hypoxia-Inducible Factor-1α (HIF-1α) and Vascular Endothelial Growth Factor (VEGF). Metformin has demonstrated its ability to reduce the incidence of cancer in diabetic patients with positive results especially in breast cancer, inhibiting cell growth by AMPK/Akt/mTOR signaling pathway. Likewise, LY294002 is the major inhibitor of PI3K/AKT/mTOR signaling pathway that has anti-angiogenic properties, capable to reduce the release of growth factors such as VEGF. The treatment with metformin in addition to the inhibitor LY294002 in both normal oxygen and hypoxia conditions, as well as the action in the process of angiogenesis in canine mammary tumors is unprecedented. Objectives: To evaluate the influence of metformin and LY294002 inhibitor treatment in tumor angiogenesis as a therapeutic strategy in mammary tumors in a in vitro and in vivo study. Material and Methods: In the in vitro study, we analyzed the cell viability of canine mammary tumor cell lines CMT-U229 (benign mixed tumor) and CF41 (metastatic carcinoma) before and after treatment with metformin and/or LY294002 by MTT assay. The cell cycle distribution was analyzed by flow cytometry flow, protein and gene expression of VEGF and HIF-1α by immunohistochemistry and RT-PCR, respectively. All experiments were performed in normal oxygen conditions and under hypoxia by the addition of cobalt chloride (CoCl2). For the in vivo study, CF41 cells were implanted in 20 female mice BALB / c nude nude. After 28 days of treatment with metformin and LY294002, it was analyzed micro vessel density by CD31 expression by immunohistochemistry as well as gene and protein expression of HIF-1α and VEGF in the tumor tissue. Results: The treatment with metformin and LY294002 was able to reduce the cellular viability after 24 hours. The protein and gene expression of HIF-1α and VEGF decreased after treatment with metformin and LY294002, both in normal oxygen conditions and hypoxia. In the in vivo study, there was a decrease in tumor size, protein and gene expression of HIF-1α and VEGFA, in addition to the decreasing of CD31 expression after all treatments. Conclusions: Our results demonstrated the effective action of metformin and LY294002 inhibitor in controlling the angiogenesis process in mammary tumors by the angiogenic factors VEGF and HIF-1α.
Introdução: A hipóxia é um conhecido fator adverso ao tratamento do câncer, capaz de ativar as vias de sinalização PI3K e MAPK/Akt/mTOR, as duas principais vias envolvidas no processo de angiogênese. Esse processo é regulado por inúmeros fatores, sendo os mais importantes o Fator Induzido por Hipóxia-1α (HIF-1α) e o Fator de Crescimento Endotelial Vascular (VEGF). A metformina tem demonstrado sua capacidade de diminuir a incidência de neoplasias em pacientes diabéticos com resultados positivos especialmente no câncer de mama, inibindo o crescimento celular através da via de sinalização MAPK/Akt/mTOR. Da mesma forma, o LY294002 é um importante inibidor da via de sinalização PI3K/AKT/mTOR que possui propriedades anti-angiogênicas, capaz de diminuir a liberação de fatores de crescimento como o VEGF. A combinação do tratamento com metformina e com o inibidor LY294002 tanto em condições normais de oxigênio quanto em hipóxia, bem como a ação no processo de angiogênese em tumores mamários caninos é inédita. Objetivos: Avaliar a influência do tratamento com metformina e com o inibidor LY294002 na angiogênese tumoral como estratégia terapêutica nas neoplasias mamárias, em um estudo in vitro e in vivo. Material e Métodos: No estudo in vitro, foi analisada a viabilidade das células das linhagens tumorais mamárias caninas CMT-U229 (tumor misto benigno) e CF41 (carcinoma metastático) antes e após o tratamento com metformina e/ou LY294002 por ensaio MTT. A distribuição das células nas fases do ciclo celular foi avaliada por citometria de fluxo, a expressão proteica e gênica do VEGF e do HIF-1α por imuno-histoquímica e PCR em Tempo Real, respectivamente. Todos os experimentos foram realizados em condições normais de oxigênio e sob hipóxia pela adição de cloreto de cobalto (CoCl2). Para o estudo in vivo, células da linhagem tumoral mamária canina CF41 foram implantadas em 20 camundongos fêmeas Balb/c nude atímicos. Após 28 dias de tratamento com metformina e LY294002, foi analisada a microdensidade vascular pela expressão do CD31 por imunohistoquímica, bem como a expressão proteica e gênica do VEGF e HIF-1α no tecido tumoral. Resultados: O tratamento com metformina e com LY294002 foi capaz de diminuir significativamente a viabilidade celular, após 24 horas. A expressão proteica e gênica do HIF-1α e do VEGF diminuiu após o tratamento com metformina e LY294002 tanto em hipóxia quanto em condições normais de oxigênio. No estudo in vivo, houve diminuição do tamanho tumoral e da expressão proteica e gênica do VEGFA e HIF-1α, além da diminuição da expressão do CD31, após os tratamentos. Conclusões: Nossos resultados demonstram a efetiva ação da metformina e do inibidor LY294002 no controle do processo de angiogênese em câncer de mama, por meio dos marcadores angiogênicos VEGF e HIF-1α.