Bronchial Carcinoids

Granberg, Dan

January 2001

<p>Bronchial carcinois are subdivided into typical and atypical. Atypical carcinoids are more malignant, but typical carcinoids may also influence survival. In the present study immunohistochemistry was performed to identify prognostic markets in patients with typical bronchial carcinoids. The diagnostic efficacy of octreoscan was evaluated, in comparison with CT and bone scan, and finally our experience of treating patients with metastatic bronchial carcinoids is reported. In an unselected material of 43 patients with typical bronchial carcinoids, metastatic disease was found in 12 patients (28%). Five patients (12%) developed distant metastases and died from their disease. High Ki-67 index, as well as positive staining for bcl-2 or p53 was associated with de- creased survival time. Positive staining for CD44s, v7-8 and v9, as well as positive nuclear staining for nm23 correlated to decreased mortality. Staining for CD44 and Ki-67 should be performed routinely for prognostic evaluation in these patients. </p><p>Octreoscan positive tumors were found in altogether 20/28 patients (71%). The primary tumor was detectable in 81% and intrathoracic metastases in 78% of the patients on octreoscan; the corresponding figures for CT were 94% and 89% respectively. Liver metastases, as shown by CT, were demonstable by octreoscan in 64% of patients. Octreoscan showed 70% and bone scan 90% sensitivity for identification of bone metastases. </p><p>Plasma chromogranin A was elevated in 28/30 patients (94%) with metastatic bronchial carcinoids and was the most sensitive tumor marker. Increased urinary 5'HIAA was found in 68%. </p><p>Biotherapy with α-interferon and Octreotide relieved carcinoid syndrome in 7/16 patients. However, only 4/27 patients showed stable disease during median 15 months, while 23 patients progressed. Treatment with cisplatinum + etoposide resulted in an objective response or stable disease for 6-8 months in 3/8 patients with widespread tumors. Doxorubicin combined with streptozotocin or paclitaxel was associated with stable disease for 9 months in 2/2 patients each. All 7 patients treated with streptozotocin+5-FU progressed. </p><p>Among the 43 unselected typical bronchial carcinoid patients, 5-year and 10-year survival was 95% and 91%, respectively. The prognosis in patients with bronchial carcinoids showing distant metastases was poor: 5-year survival was 70% from diagnosis and 22% from treatment start. </p>

Medical sciences

Bronchial carcinoids

immunohistochemistry

prognostic markers

diagnosis

octreoscan

circulating hormones

treatment

MEDICIN OCH VÅRD

MEDICINE

MEDICIN

Bronchial Carcinoids

Granberg, Dan

January 2001

Bronchial carcinois are subdivided into typical and atypical. Atypical carcinoids are more malignant, but typical carcinoids may also influence survival. In the present study immunohistochemistry was performed to identify prognostic markets in patients with typical bronchial carcinoids. The diagnostic efficacy of octreoscan was evaluated, in comparison with CT and bone scan, and finally our experience of treating patients with metastatic bronchial carcinoids is reported. In an unselected material of 43 patients with typical bronchial carcinoids, metastatic disease was found in 12 patients (28%). Five patients (12%) developed distant metastases and died from their disease. High Ki-67 index, as well as positive staining for bcl-2 or p53 was associated with de- creased survival time. Positive staining for CD44s, v7-8 and v9, as well as positive nuclear staining for nm23 correlated to decreased mortality. Staining for CD44 and Ki-67 should be performed routinely for prognostic evaluation in these patients. Octreoscan positive tumors were found in altogether 20/28 patients (71%). The primary tumor was detectable in 81% and intrathoracic metastases in 78% of the patients on octreoscan; the corresponding figures for CT were 94% and 89% respectively. Liver metastases, as shown by CT, were demonstable by octreoscan in 64% of patients. Octreoscan showed 70% and bone scan 90% sensitivity for identification of bone metastases. Plasma chromogranin A was elevated in 28/30 patients (94%) with metastatic bronchial carcinoids and was the most sensitive tumor marker. Increased urinary 5'HIAA was found in 68%. Biotherapy with α-interferon and Octreotide relieved carcinoid syndrome in 7/16 patients. However, only 4/27 patients showed stable disease during median 15 months, while 23 patients progressed. Treatment with cisplatinum + etoposide resulted in an objective response or stable disease for 6-8 months in 3/8 patients with widespread tumors. Doxorubicin combined with streptozotocin or paclitaxel was associated with stable disease for 9 months in 2/2 patients each. All 7 patients treated with streptozotocin+5-FU progressed. Among the 43 unselected typical bronchial carcinoid patients, 5-year and 10-year survival was 95% and 91%, respectively. The prognosis in patients with bronchial carcinoids showing distant metastases was poor: 5-year survival was 70% from diagnosis and 22% from treatment start.

Medical sciences

Bronchial carcinoids

immunohistochemistry

prognostic markers

diagnosis

octreoscan

circulating hormones

treatment

MEDICIN OCH VÅRD

MEDICINE

MEDICIN

Vztah nádorového genotypu a fenotypu k diagnostice, prognóze a predikci kolorektálního karcinomu / Relation of tumor genotype and phenotype to diagnosis, prognosis and prediction of colorectal cancer

Pitule, Pavel

January 2014

Colorectal cancer is one of the most common type of malignity. Despite of the existence of numerous studies focused on this carcinoma, there are still many unknown features regarding its diagnosis, treatment or prognosis. In the thesis we focused on the identification of novel prognostics markers that could be useful for the stratification of patients based on the disease outcomes. In the first study we immunohistochemically assessed expression of two proteins associated with cancer stem cells in the samples of primary colorectal cancer and matched liver metastasis. Goal of the study was to evaluate relation among expression of CD44 and CD133 and overall survival and disease free interval in our set of patients. We observed that increased ratio of CD133 positive compared to CD133 negative tumor glands resulted in longer disease free interval, finding which is opposite to the general view on the CD133 role in the cancer development. Our hypothesis is that we analyzed confined group of patients and followed a bit different goal, where we measured ratio between positive and negative glands in the view-field and not the intensity of staining as the previous studies did. Our second study was focused on the transcriptional analysis of the selected set of twelve genes using frozen samples from colorectal...

Prognostic markers and DNA methylation profiling in lymphoid malignancies

Bhoi, Sujata

January 2017

In recent years, great progress has been achieved towards identifying novel biomarkers in lymphoid malignancies, including chronic lymphocytic leukemia (CLL) and mantle cell lymphoma (MCL), at the genomic, transcriptomic and epigenomic level for accurate risk-stratification and prediction of treatment response. In paper I, we validated the prognostic relevance of a recently proposed RNA-based marker in CLL, UGT2B17, and analyzed its expression levels in 253 early-stage patients. Besides confirming its prognostic impact in multivariate analysis, we could identify 30% of IGHV-mutated CLL (M-CLL) cases with high expression and poor outcome, which otherwise lacked any other poor-prognostic marker. In paper II, we investigated the prognostic impact of a previously reported 5 CpG signature that divides CLL patients into three clinico-biological subgroups, namely naive B-cell-like CLL (n-CLL), memory B-cell-like CLL (m-CLL) and intermediate CLL (i-CLL), in 135 CLL patients using pyrosequencing. We validated the signature as an independent marker in multivariate analysis and further reported that subset #2 cases were predominantly classified as i-CLL, although displaying a similar outcome as n-CLL. In paper III, we investigated the methylation status and expression level of miR26A1 in both CLL (n=70) and MCL (n=65) cohorts. High miR26A1 methylation was associated with IGHV-unmutated (U-CLL) and shorter overall survival (OS) in CLL, while it was uniformly hypermethylated in MCL. Furthermore, overexpression of miR26A1 resulted in significant downregulation of EZH2 that in turn led to increased apoptosis. In paper IV, we performed DNA methylation profiling in 176 CLL cases assigned to one of 8 major stereotyped subsets (#1-8) in relation to non-subset CLL (n=325) and different normal B-cell subpopulations. Principal component analysis of subset vs. non-subset CLL revealed that U-CLL and M-CLL subsets generally clustered with n-CLL and m-CLL, respectively, indicating common cellular origins. In contrast, subset #2 emerged as the first defined member of the i-CLL subgroup, which in turn alludes to a distinct cellular origin for subset #2 and i-CLL patients. Altogether, this thesis confirms the prognostic significance of RNA and epigenetic-based markers in CLL, provides insight into the mechanism of miRNA deregulation in lymphoid malignancies and further unravels the DNA methylation landscape in stereotyped subsets of CLL.

Lymphoid malignancies

CLL

MCL

prognostic markers

micro-RNA

methylation

stereotyped subsets

Hematology

Hematologi

Vztah nádorového genotypu a fenotypu k diagnostice, prognóze a predikci kolorektálního karcinomu / Relation of tumor genotype and phenotype to diagnosis, prognosis and prediction of colorectal cancer

Pitule, Pavel

January 2014

Colorectal cancer is one of the most common type of malignity. Despite of the existence of numerous studies focused on this carcinoma, there are still many unknown features regarding its diagnosis, treatment or prognosis. In the thesis we focused on the identification of novel prognostics markers that could be useful for the stratification of patients based on the disease outcomes. In the first study we immunohistochemically assessed expression of two proteins associated with cancer stem cells in the samples of primary colorectal cancer and matched liver metastasis. Goal of the study was to evaluate relation among expression of CD44 and CD133 and overall survival and disease free interval in our set of patients. We observed that increased ratio of CD133 positive compared to CD133 negative tumor glands resulted in longer disease free interval, finding which is opposite to the general view on the CD133 role in the cancer development. Our hypothesis is that we analyzed confined group of patients and followed a bit different goal, where we measured ratio between positive and negative glands in the view-field and not the intensity of staining as the previous studies did. Our second study was focused on the transcriptional analysis of the selected set of twelve genes using frozen samples from colorectal...

Identification of Prognostically Relevant Cellular Markers of Differentiation in Glioblastoma

Behling, Felix

27 September 2016

No description available.

610

Glioblastoma

Immunohistochemistry

Prognostic Markers

OLIG2

P53

NogoA

GFAP

Ki67

Overall Survival

IDH1

Medizin (PPN619874732)

Histopathologie {Medizin} (PPN619875704)

Valeur pronostique du remodelage de la signalisation calcique dans le cancer de la prostate / Prognostic value of Calcium signalling remodelling in prostate cancer

Perrouin-Verbe, Marie-Aimée

22 December 2017

Le cancer de prostate (CaP) est le plus fréquent chez l’homme de plus de 50 ans. La généralisation du PSA et du dépistage du CaP a permis son diagnostic à des formes localisées (80% des formes diagnostiquées), accessibles à un traitement curatif. De plus, un certain nombre de ces formes localisées sont indolentes, de très faible risque, éligibles à une surveillance active (SA).Cependant, 15 à 25% des patients vont présenter une récidive 10 ans après un traitement curatif, et environ 30% des patients inclus en SA seraient en fait sous-évalués (cancer significatif). Il est donc nécessaire d’identifier de nouveaux biomarqueurs pronostiques capables de distinguer les tumeurs indolentes des tumeurs à haut risque, et capables d’améliorer la prédiction du risque de récidive après traitement curatif. Objectifs : Evaluer la valeur pronostique potentielle du remodelage de la signalisation calcique dans le cancer de prostate : 1) Evaluer le lien entre remodelage de la signalisation calcique et agressivité tumorale 2) Evaluer l’impact pronostique du remodelage de la signalisation calcique sur la récidive systémique après prostatectomie radicale(PR). 3) Evaluer l’apport du remodelage de la signalisation calcique dans la sélection des patients éligibles à la surveillance active. Méthodologie 1) Evaluation de l’expression (immunohistochimie) de TRPC1, TRPC4, Orai1 et STIM1 à différents stades de progression du CaP, et évaluation de l’impact pronostique de cette expression sur la récidive dans le CaP localisé à partir d’une cohorte de 238 patients. 2) Etude cas-témoin à partir d’une cohorte de 112 patients opérés d’un CaP localisé. Evaluation de l’impact pronostique de l’expression (immunohistochimie) de 10 acteurs de la signalisation calcique (Orai1, Orai2, Orai3, STIM1, STIM2, TRPV5 et V6, TRPC1 et C4, TRPM8) sur la récidive systémique après PR. 3). A partir d’une cohorte de patients ayant été opérés pour des cancers de faible risque, ont été inclus les patients potentiellement éligibles à une SA au moment du diagnostic (n=71). Etude de l’apport de la signalisation calcique dans la sélection des patients éligibles à la SA (marquage immunohistochimie sur biopsies et pièce opératoire : TRPC1 et C4, TRPV5 et V6, Orai1, STIM1) Résultats 1) Dans le Cap localisé, une surexpression de TRPC1 était associée à une prolifération plus faible et une meilleure survie sans récidive (indépendant des marqueurs pronostiques usuels). 2) Une surexpression de TRPC4, TRPV5 et TRPV6 est associée à un plus faible risque de récidive systémique après prostatectomie, et ce indépendamment des 5 facteurs pronostiques usuels. 3) Un marquage plus intense de TRPV6 sur les biopsies prostatiques semble associé à un CaP significatif, éligible à un traitement curatif d’emblée chez les patients présentant un CaP de faible risque. Conclusion : Sur pièce de PR, TRPC1, TRPC4, TRPV5 et TRPV6 possèdent une valeur pronostique indépendante et sont associés à un plus faible risque de récidive après PR. Sur biopsie prostatique, TRPV6 permet de distinguer les CaP indolents des significatifs chez les patients présentant un CaP de faible risque. / Prostate cancer (PCa) is the most common malignancy in men 50 years and older and the second leading cause of cancerrelated death in men in developed countries. Widespread PSA screening has allowed an increase rate of localised PCa at diagnosis, managed by curative treatment such as radical prostatectomy (RP), or active surveillance (AS) in case of indolent disease. However, 30% of patients experience biochemical relapse during the 10 years following RP. Moreover, 30% of patients in AS are undervalued and present a significant disease. It is therefore necessary to identify new prognostic biomarkers capable of distinguishing indolent from significant tumours, and capable to accurately predict the risk of recurrence after curative treatment. Objectives: To evaluate the potential prognostic value of calcium signalling remodeling in PCa: 1) To assess the impact of calcium signalling remodelling on tumour aggressiveness 2) To assess the prognostic value of calcium signalling remodelling on systemic recurrence after RP. 3) To assess the contribution of calcium signaling remodelling in the selection of patients for active surveillance (AS). Methods 1) Study of the expression (immunohistochemistry) of TRPC1, TRPC4, Orai1 and STIM1 at different stages of PCa, and assessment of the prognostic value of this expression on recurrence in clinically localised PCa (CLC) in a cohort of 238 patients. 2) Case-control study on a cohort of 112 patients who underwent RP for CLC. Evaluation of the prognostic impact of the expression (immunohistochemistry) of 10 actors of calcium signalling (Orai1, Orai2, Orai3, STIM1, STIM2, TRPV5 and V6, TRPC1 and C4, TRPM8) on systemic recurrence after RP. 3) From a cohort of patients who underwent RP for low-risk PCa, were enrolled patients potentially eligible for AS at the time of diagnosis (n = 71). We evaluated the impact of calcium signalling remodelling in patients selection for AS (immunohistochemical staining on biopsies and prostate specimens: TRPC1 and C4, TRPV5 and V6, Orai1, STIM1).Results 1) In CLC, an overexpression of TRPC1 was associated with a decreased proliferation, and with a higher rate of biochemical progression-free survival (independent of usual prognostic markers). 2) Overexpression of TRPC4, TRPV5 and TRPV6 was associated with a lower risk of systemic recurrence after RP, independently of the prognostic factors currently used. 3) More intense staining of TRPV6 on biopsies was associated with a significant PCa, for which a curative treatment is required. Conclusion: On RP specimens, overexpression of TRPC1, TRPC4, TRPV5 and TRPV6 has an independent prognostic value and is associated with a lower risk of recurrence after RP. On prostate biopsies, TRPV6 allows to distinguish indolent from significant disease in patients with low-risk PCa.

Cancer de prostate

Marqueurs pronostiques

Récidive

Surveillance active

Signalisation calcique

Prostate cancer

Prognostic markers

Recurrence

Active surveillance

Calcium signalling

616.994 63

Patologia molecular dos tumores mamário caninos : expressão de marcadores prognósticos e mioepiteliais

Motta, Adriana Costa da

January 2008

Os marcadores prognósticos em mastologia têm sido utilizados como apoio diagnóstico para prever o comportamento dos neoplasmas mamários (prognóstico) e determinar a provável resposta ao tratamento pré ou pós-cirúrgico. Estudos têm sido feitos sobre o prognóstico dos tumores mamários caninos (TMCs) que apresentam semelhanças e diferenças com tumores mamários humanos. Além disso, esses tumores exibem, com alta freqüência, proliferação de células mioepiteliais que podem sofrer metaplasia, acompanhada de alterações moleculares. O presente estudo teve o objetivo de verificar a expressão imuno-histoquímica e a associação de diferentes marcadores utilizados como prognósticos nos tumores de mama humana (RE, RP, c-erbB-2 e Ki-67) e marcadores mioepiteliais (p63, CK5 e vimentina) nos TMCs. O primeiro artigo analisa a expressão desses marcadores em 35 tumores encontrados em onze fêmeas caninas nas quais foram identificados tumores malignos múltiplos nas glândulas mamárias. Cada tipo histológico analisado em fêmeas portadoras de tumores múltiplos expressou marcadores prognósticos e mioepiteliais peculiares à sua histogênese, porém houve associação dessa expressão apenas em alguns tipos celulares presentes nos TMCs. Os tumores com componente epitelial carcinomatoso não apresentaram diferenças significativas, no entanto, nos tumores com componente complexo e misto, ocorreu associação entre a expressão da p63, CK5 e vimentina. No conjunto de marcadores estudados, a p63 e a CK5 mostram-se promissoras na elucidação da transformação das células mioepiteliais concomitante à invasão tumoral e com relação à expressão da vimentina que se mostrou bem evidenciada durante a transformação da célula mioepitelial proliferada a célula participante do mesênquima do neoplasma invasor em mamas de caninos, ao menos nos aspectos de expressão molecular e morfológica. O segundo artigo analisa os marcadores mioepiteliais em 82 casos de TMCs malignos. Este estudo comprovou a freqüência e a associação da expressão desses marcadores em determinados tipos histológicos tumorais e celulares, permitindo a identificação das células mioepiteliais em transformação na maior parte dos TMCs malignos, notadamente, os que apresentam componente mesenquimal metaplásico. Mais estudos devem ser feitos na tentativa de verificar a significância da expressão encontrada no comportamento biológico desses tumores. / Prognostic markers in mastology have been used as diagnostic support, to predict the behavior of mammary neoplasias (prognosis) and to determine their possible response to treatment before or after surgery. Studies have been conducted on the prognosis of canine mammary gland tumors (MGTs), which show similarities to and differences from human breast tumors. In addition, these tumors often show proliferation of myoepithelial cells, which may undergo metaplasia, accompanied by molecular alterations. The aim of the present study was to check the immunohistochemical expression and the association between different markers used as prognostic factors in human breast tumors (ER, RP, c-erbB-2 and Ki-67) and myoepithelial markers (p63, CK5 and vimentin) in MGTs. The first article analyzes the expression of these markers in 35 tumors in 11 female dogs, where multiple tumors were identified in the mammary glands. Each histological type analyzed in the female dogs with multiple tumors expressed prognostic and myoepithelial markers that were peculiar to their histogenesis, but the association of this expression was observed only in some cell types of MGTs. Tumors with a carcinomatous epithelial component did not have significant differences, but tumors with complex and mixed components showed association between the expressions of p63, CK5 and vimentin. Of the group of investigated markers, p63 and CK5 proved to be promising tools in elucidating the transformation of myoepithelial cells concomitantly to tumor invasion and in terms of vimentin expression, which was quite pronounced in this transformation from proliferating myoepithelial cells into cells that participate in the mesenchyma of the invasive neoplasia in canine mammary glands, at least with regard to the aspects of molecular and morphological expression. The second article analyzes myoepithelial markers in 82 cases of malignant MGTs. This study corroborated the frequency and association of the expression of these markers in certain histological tumor and cell types, allowing for the identification of myoepithelial cells in transformation in most malignant MGTs, chiefly those with a metaplastic mesenchymal component. Further studies are necessary in order to assess the importance of expression found in the biological behavior of these tumors.

Neoplasias da mama

Biomarcadores tumorais

Modelos animais de doenças

Cães

Mioepitelioma

Prognostic markers

Myoepithelial markers

Immunohistochemistry

Mammary neoplasms

Dog

RNA-based Prognostic Markers in Chronic Lymphocytic Leukemia

Sevov, Marie

January 2010

Chronic lymphocytic leukemia (CLL) is a heterogeneous disease where a significant proportion of patients will develop an aggressive disease. Today, the mutational status of the immunoglobulin heavy variable (IGHV) genes is one of the strongest prognostic markers in CLL, where unmutated IGHV genes correlate with poor outcome. In addition, IGHV3-21 gene usage is associated with poor prognosis independent of mutational status. Recently, several genes were shown to be differently expressed between IGHV mutated and unmutated CLL and were suggested as prognostic markers. The aim of this thesis was to examine the applicability of these RNA-based prognostic markers in CLL. In papers I and II, the prognostic significance of LPL and TCL1A mRNA expression in CLL was investigated in 140 and 144 patients, respectively. High expression was found to be associated with inferior clinical outcome for both markers. However, CLL cases with mutated IGHV3-21 genes displayed low levels of LPL expression, indicating that LPL cannot identify this poor-risk patient group. In contrast, high TCL1A expression was detected in all IGHV3-21 cases. To elucidate the functionality of LPL in CLL, LPL lipase activity was measured in 33 cases. The lipase activity was found to be invariably low, implying an alternative function for LPL in CLL. In paper III, a comprehensive analysis of five RNA-based markers (LPL, TCL1A, ZAP70, CLLU1 and MCL1) was performed in 252 CLL patients. All RNA-based markers except MCL1 predicted clinical outcome, with LPL being the strongest. Moreover, LPL expression independently predicted overall survival when adjusted for established markers. All of the RNA-based markers added additional prognostic information to established markers, e.g. high LPL expression predicted an inferior outcome in patients with mutated IGHV genes or good-risk cytogenetics. For clinical application, over time stability of prognostic markers is crucial. In paper IV, the expression of LPL, TCL1A, ZAP70 and MCL1 was investigated in samples taken at diagnosis and at a follow-up of seven years in 104 CLL patients. LPL was found to be the most stable marker, displaying high correlation between the sequential samples, whereas ZAP70 and MCL1 varied significantly. TCL1A expression increased at follow-up, which may indicate disease progression as TCL1A promotes cell survival. In summary, this thesis highlights the applicability of RNA-based markers in CLL prognostication, both as single markers or in combination with established markers. In particular, LPL was shown to be the strongest RNA-based marker in terms of prognostic strength and stability.

Chronic lymphocytic leukemia

prognostic markers

RNA-based markers

LPL

Haematology

Hematologi

Les thérapies anti-angiogéniques : entre espoir et réalité. Vers l'identification de marqueurs prédictifs et de nouvelles cibles thérapeutiques dans le traitement du cancer du rein / The anti-angiogenic therapy : between hope and reality. Toward the identification of predictive markers and new therapeutic targets in renal cancer

Guyot, Mélanie

19 July 2013

L’ensemble de ce travail vise à étudier les mécanismes de résistance aux thérapies anti-angiogéniques dans le traitement du cancer du rein à cellules claires (ccRCC). Nous avons mis en évidence que le bévacizumab (BVZ), un anticorps monoclonal humanisé anti-VEGF utilisé en clinique, accélère la croissance de ccRCC humain chez la souris nude. Ce modèle mime la phase d’échappement souvent observée chez les patients. Le traitement BVZ induit de la lymphangiogenèse associée à une surexpression du VEGF-C. Les cellules tumorales après traitement possèdent également des capacités d’invasion accrues. Ainsi, le traitement BVZ pourrait faciliter la progression tumorale et la formation de métastases dans les ccRCC. Le traitement entraine également une diminution de l’expression d’une phosphatase membranaire, la phospho-tyrosine phosphatase récepteur kappa (PTPR)impliquée dans le contrôle de l’activité de récepteurs à activité tyrosine kinase, comme le récepteur de l’EGF, du PDGF et de l’HGF. Ces récepteurs régulent la prolifération et la migration cellulaire. Le traitement BVZ faciliterait donc la croissance tumorale indépendante du VEGF. Enfin, le traitement induit une augmentation de la sécrétion de cytokines angiogéniques redondantes qui prennent le relais du VEGF, comme les cytokines CXCL7 et CXCL8, et facilitent le développement tumoral sous traitement BVZ. En particuliers, la cytokine CXCL7 et ses récepteurs CXCR1-2 ont un rôle central dans le développement des ccRCC. Cibler l’axe CXCL7/CXCR1-2 réduit efficacement la croissance tumorale. Les récepteurs cibles de PTPR, pour lesquels des inhibiteurs sont actuellement utilisés pour le traitement d’autres cancers, le VEGF-C et la cytokine CXCL7, pourraient donc constituer de nouveaux marqueurs prédictifs d’efficacité du BVZ et de nouvelles cibles thérapeutiques dans le traitement des ccRCC. La résistance au BVZ pourrait également s’expliquer par l’existence de formes "bénéfiques" anti-angiogéniques du VEGF qui sont reconnues par le BVZ avec la même affinité que les formes pro-angiogéniques. Nous avons mis en évidence qu’une immunisation prophylactique à l’aide d’un peptide spécifique du VEGF pro-angiogénique limite la croissance tumorale de ccRCC syngéniques de souris. De la même façon, en traitement curatif, l’utilisation d’anticorps spécifiques du VEGF pro-angiogénique bloque la croissance de ccRCC chez la souris nude sans induire les différents mécanismes d’échappement observés avec le BVZ. Ces résultats suggèrent la pertinence du ciblage spécifique des formes pro-angiogéniques de VEGF dans le traitement des ccRCC. / The aim of my work is to study resistance mechanisms to anti-angiogenic treatments of Clear Cell Renal Carcinoma (ccRCC). We observed that bevacizumab (BVZ) -a humanized monoclonal antibody targeting VEGF and currently used in the clinic- promotes the growth of human ccRCC xenografts in nude mice. This model mimics the “escape phase” widely observed in patients. BVZ treatment induces lymphangiogenesis and over-expression of VEGF-C. Tumor cells exposed to the treatment acquire an increased spreading capacity. Hence, BVZ might promote tumor progression and metastasis formation of ccRCC. Furthermore, this treatment decreases the expression of the receptor phosphor tyrosine phosphatase kappa (PTRP). This phosphatase is involved in the regulation of tyrosine kinase receptors controlling growth and migration, among others EGF, PDGF and HGF receptors. Thus, BVZ might promote tumor growth independently of VEGF. Moreover, the treatment increases secretion of redundant cytokines like CXCL7 and CXCL8. By their ability to exert similar effect as VEGF, these cytokines promote tumor development under BVZ treatment. In particular, CXCL7 and its receptors CXCR1 and CXCR2, play a central role in the development of ccRCC. Targeting this pathway efficiently reduces tumor growth. Target receptors of PTRP for which inhibitors are currently used for other cancers, VEGF-C and CXCL7 could therefore be regarded as new predictive markers for BVZ efficiency and may be considered as potential therapeutic targets. Resistance to BVZ could also be explained by the presence of "beneficial" forms of anti-angiogenic VEGF recognized by the BVZ with the same affinity as the pro-angiogenic forms. We have demonstrated that prophylactic immunization with a pro-angiogenic VEGF-specific peptide limits tumor growth of murine syngeneic ccRCC. Similarly, in curative therapy, antibodies specific for pro-angiogenic VEGF block growth of ccRCC in nude mice without inducing the escape mechanisms observed with BVZ. These results highlight the relevance of targeting such pro-angiogenic forms of VEGF for the treatment of ccRCC.

Angiogenèse

Traitements anti-angiogéniques

Résistances

CcRCC

Marqueurs prédictifs et pronostiques

Angiogenesis

Anti-angiogenic therapy

Resistance

CcRCC

Predictive and prognostic markers