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1	Anaplastic Thyroid Carcinoma Arising in Long-Standing Multinodular Goiter Following Radioactive Iodine Therapy: Report of a Case Diagnosed by Fine Needle Aspiration Maatouk, Jamal, Barklow, Thomas A., Zakaria, Wael, Al-Abbadi, Mousa A. 01 January 2009 (has links) Background: Anaplastic thyroid carcinoma (ATC) is a highly aggressive, undifferentiated carcinoma that may arise on top of normal or abnormal thyroid. Making the diagnosis by fine needle aspiration (FNA) of the thyroid with a long-standing history of multinodular goiter (MNG) is not uncommon. We report a case discussing the cytopathologic findings and the relationship with long-standing goiter and thyroid exposure to radioactive iodine treatment. Case: A 90-year-old male patient presented with a > 45-year history of MNG that was associated with thyrotoxicosis and multiple courses of radioiodine (I-131) treatment. He developed recent symptoms of dyspnea, dysphagia, neck swelling and unintentional weight loss. Computed tomography of the neck was done revealing a large MNG with retrosternal extension and calcifications. FNA was performed revealing highly anaplastic cells with a colloid background and presence of neutrophils. The diagnosis of ATC was made. The patient refused any kind of management and was discharged upon his request. He died 2 days after the procedure, and no autopsy was performed. Conclusion: ATC is an aggressive, undifferentiated thyroid carcinoma that can be diagnosed by FNA and save the patient a surgical intervention. A background of MNG and history of radioactive iodine therapy is not uncommon. anaplastic thyroid carcinoma aspiration biopsy fine-needle carcinoma anaplastic nodular goiter thyroid cancer Pathology
2	TKI sensitivity patterns of novel kinase-domain mutations suggest therapeutic opportunities for patients with resistant ALK+ tumors Amin, Amit Dipak, Li, Lingxiao, Rajan, Soumya S., Gokhale, Vijay, Groysman, Matthew J., Pongtornpipat, Praechompoo, Tapia, Edgar O., Wang, Mengdie, Schatz, Jonathan H. 25 April 2016 (has links) The anaplastic lymphoma kinase (ALK) protein drives tumorigenesis in subsets of several tumors through chromosomal rearrangements that express and activate its C-terminal kinase domain. In addition, germline predisposition alleles and acquired mutations are found in the full-length protein in the pediatric tumor neuroblastoma. ALK-specific tyrosine kinase inhibitors (TKIs) have become important new drugs for ALK-driven lung cancer, but acquired resistance via multiple mechanisms including kinase-domain mutations eventually develops, limiting median progression-free survival to less than a year. Here we assess the impact of several kinase-domain mutations that arose during TKI resistance selections of ALK+ anaplastic large-cell lymphoma (ALCL) cell lines. These include novel variants with respect to ALK-fusion cancers, R1192P and T1151M, and with respect to ALCL, F1174L and I1171S. We assess the effects of these mutations on the activity of six clinical inhibitors in independent systems engineered to depend on either the ALCL fusion kinase NPM-ALK or the lung-cancer fusion kinase EML4-ALK. Our results inform treatment strategies with a likelihood of bypassing mutations when detected in resistant patient samples and highlight differences between the effects of particular mutations on the two ALK fusions. anaplastic lymphoma kinase drug resistance crizotinib ceritinib alectinib
3	Neuroblastome, résistance in vivo à l'irinotecan et voie de signalisation ALK / Neuroblastoma, in vivo resistance to irinotecan and ALK signaling pathway Bousseton, Munier 07 June 2012 (has links) Les neuroblastomes, même de haut risque répondent bien à la chimiothérapie initiale mais deviendront fréquemment résistants au traitement. Les inhibiteurs de topoisomérase I représentent un outil thérapeutique important dans la prise en charge des neuroblastomes réfractaires. Pour étudier la résistance aux inhibiteurs de topoisomérase I acquise dans un contexte thérapeutique, un modèle murin de neuroblastome résistant au CPT-11 a été développé. La chimiorésistance est connue comme un phénomène multifacoriel. Nous avons donc utilisé plusieurs approches pour mieux caractériser les mécanismes à l'origine de la résistance dans notre modèle. Une approche génomique a permis d'identifier la dérégulation de la voie de signalisation formée du récepteur ALK et de deux ligands PTN et MDK. Alors que ALK est décrit comme gène majeur de prédisposition au neuroblastome, principalement par le biais de mutations activatrices, nous avons démontré que l'activation du récepteur survenait par des mécanismes alternatifs aux mutations dans une large majorité de cas et participerait à l'initiation de la maladie. En revanche, nous n'avons pas pu prouver l'implication de ce récepteur dans la progression de la maladie ou dans sa réponse au traitement. Il semble que la régulation de ALK soit complexe et le rôle exact de ce récepteur dans la progression du neuroblastome reste à établir. En revanche, nous avons démontré l'importance du ligand MDK dans la régulation de l'expression et de l'activation de ALK ainsi que dans le contrôle de la survie des cellules neuroblastiques. Inhiber cette cytokine représente une stratégie thérapeutique intéressante, complémentaire des thérapies anti-ALK, actuellement en développement clinique dans le neuroblastome. D’autre part, la caractérisation phénotypique du modèle a permis de mettre en évidence une signalisation altérée des dommages à l'ADN associée à une instabilité génétique accrue dans les tumeurs résistantes. Celles-ci présentent également une modification de progression dans le cycle cellulaire et une proportion plus importante de cellules quiescentes. Au final, ce travail a permis d'identifier différents mécanismes de résistance qui représentent des marqueurs de réponse au traitement et des cibles thérapeutiques intéressantes dans le neuroblastome. / Neuroblastoma, including high-risk cases, show a good initial response to chemotherapy but will frequently become resistant to treatment. Topoisomerase I inhibitors represent an important therapeutic option for refractory neuroblastoma. To study the reisitance to topoisomerase I inhibitors acquired in a therapeutic setting, we developed in vivo a resistant model to irinotecan (CPT-11). Chemoresistance is known as a multifactorial phenomenon. We have therefore used several approaches to better characterize mechanisms leading to resistance in our model. A genomic approach enabled us to identify the deregulation of a signaling pathway, constituted with a receptor (ALK) and two lignads (PTN and MDK). While ALK is decsribed as a major neuroblastoma predisposition gene, mainly through activating mutations, we demonstrated that the activation of ALK occurs via mechanisms others than mutation in a large majority of cases. Moreover ALK activation is an important event in the initiation of the disease. However, we couldn’t prouve the implication of the receptor in the progression of the disease or in its response to treatment. It seems that the regulation of ALK is complex and its precise role in the progression of neuroblastoma remains to be precisely defined. Nevertheless, we have demonstrated the importance of MDK, one of ALK ligands in the regulation of the expression and activation of ALK as well as in the control of the neuroblastoma cells survival. The inhibition of the cytokine, MDK represents an interesting therapeutic strategy, complementary to anti-ALK therapies, currently in clinical development in neuroblastoma. On another hand, the phenotypic characterization of the model, showed an alteration of the signaling of DNA damage and an increased genomic instability in the resistant tumors. Those tumors also harbor a modification in the cell cycle progression, particularly an increased proportion of quiescent cells. Finally, this work enables us to identify several resistance mechanism that represent markers of response to chemotherapy and relevant therapeutic targets in neuroblastoma. Neuroblastome Résistance Anaplastique Lymphoma Kinase Neuroblastoma Resistance Anaplastic Lymphoma Kinase
4	Pioneers of Breast Implant-Associated Anaplastic Large Cell Lymphoma: History from Case Report to Global Recognition Miranda, Roberto N., Medeiros, L. Jeffrey, Ferrufino-Schmidt, Maria C., Keech, John A., Brody, Garry S., de Jong, Daphne, Dogan, Ahmet, Clemens, Mark W. 01 March 2019 (has links) The first case of breast implant-associated anaplastic large cell lymphoma (breast implant ALCL) was described by John Keech and the late Brevator Creech in 1997. In the following 2 decades, much research has led to acceptance of breast implant ALCL as a specific clinicopathologic entity, a process that we bring up to life through the memories of 6 persons who were involved in this progress, although we acknowledge that many others also have contributed to the current state of the art of this disease. Dr. Keech recalls the events that led him and Creech to first report the disease. Ahmet Dogan and colleagues at the Mayo Clinic described a series of 4 patients with breast implant ALCL, and led to increased awareness of breast implant ALCL in the pathology community. Daphne de Jong and colleagues in the Netherlands were the first to provide epidemiologic evidence to support the association between breast implants and ALCL. Garry Brody was one of the first investigators to collect a large number of patients with the disease, present the spectrum of clinical findings, and alert the community of plastic surgeons. Roberto Miranda and L. Jeffrey Medeiros and colleagues studied the pathologic findings of a large number of cases of breast implant ALCL, and published the findings in 2 impactful studies in the medical oncology literature. The recognition and acceptance of this disease by surgeons, epidemiologists, and medical oncologists, working together, has led to subsequent studies on the pathogenesis and optimal therapy of this disease. / Revisión por pares Adult Adverse device effect Anaplastic large cell lymphoma Breast augmentation
5	The Mystery of Multiple Masses: A Case of Anaplastic Astrocytoma Sethi, Pooja, Treece, Jennifer, Pai, Vandana, Onweni, Chidinma, Rahman, Zia, Singh, Siddharth 23 June 2017 (has links) Though most primary brain gliomas present as a single mass lesion in the brain, this potential diagnosis must be considered in the differential diagnosis when faced with a case of multifocal brain mass lesions. Among the most common brain tumors in humans, glioblastomas can be classified into four classes, one of which consists of anaplastic astrocytomas (AA). Due to its significant malignant potential, a prompt stereotactic brain biopsy should be considered to allow for early diagnosis. Karyotypic analysis of the specimen may allow for the discovery of 1p12q and IDH132 gene mutations. This knowledge can be used to best determine prognosis and guide therapy. anaplastic astrocytoma brain mass primary brain glioma Internal Medicine
6	Quantitative mikroskopische Analyse der Regulationsmechanismen der Anaplastic Lymphoma Kinase in Neuroblastomzellen / Quantitative microscopic analysis of the regulatory mechanisms of the anaplastic lymphoma kinase in neuroblastoma Schumacher, Marten 13 January 2020 (has links) No description available. 610 Neuroblastom ALK Anaplastic Lymphoma Kinase F1174 R1275 Y1604 I1250 neuroblastoma ALK anaplastic lymphoma kinase F1174 I1250 R1275 Y1604 Medizin (PPN619874732)
7	Metastasierungsverhalten und Prognose von verrukösen Karzinomen -Literaturübersicht und retrospektive Studie- Neumeyer, Rita 28 July 1998 (has links) Die Arbeit umfaßt erstens einen Literaturüberblick über die charakteristischen Merkmale und Besonderheiten des verrukösen Karzinoms (VK) und die Prognose bei unterschiedlichen therapeutischen Herangehensweisen. Von besonderem Interesse ist die LK-Metastasierung von VK. In der Literaturauswertung konnten dabei 18 Fälle ermittelt werden; dabei waren nur in einem Fall Fernmetastasen vorhanden. Die Prognose von VK ist gut bei einer adäquaten chirurgischen Therapie; die Mitbehandlung des Lymphabstromgebietes sollte nicht routinemäßig erfolgen. Zweiter Schwerpunkt der Arbeit ist eine Auswertung des Patientengutes der Klinik und Poliklinik für Mund-, Kiefer- und Gesichtschirurgie der Charité (24 Patienten) und der Hals-Nasen-Ohrenklinik der Charité (13 Patienten) unter der besonderen Fragestellung des Metastasierungsverhaltens und der Prognose von VK. In 2 Fällen wurden LK-Metastasen eines VK festgestellt. In keinem Fall ist das VK als Todesursache eines Patienten bekannt. Bei 8 Patienten traten Rezidive auf. Es wurde festgestellt, daß größere Tumoren schneller und häufiger rezidivieren. Bei der Hälfte der Patienten trat das Rezidiv 4 bis 9 Monate post operationem auf. Die Früherkennung von VK ist wichtig, denn die Prognose ist umso besser, je kleiner der Tumor ist. / The paper comprises first an assessment of literature about the characteristics, and the particularities of verrucous carcinoma (VC), and prognosis dependent on the different therapies. Of particular interest is the lymph node metastatic invasion of VC. The assessment of literature showed in 18 cases lymph node metastases; one VC of these had distant metastases. The prognosis of VC is excellent with adequate surgical therapy. Lymph node treatment should not be routine. Second point of the paper is the assessment of data of 24 patients with VC of the Clinic for Oral and Maxillo-Facial surgery of the Charité and 13 patients with VC of the Clinic for Otorhinolaryngology of the Charité with special attention on metastatic invasion and prognosis of VC. Two patients had lymph node metastases caused by a VC. In no case VC is known as cause of death. Eight patients had relapses. Half of these patients had relapse 4 to 9 monthes post operationem. It was established that larger tumors relapse more often and faster. Early detection of VC is necessary, because the prognosis is the better the smaller the tumor is. verruköses Karzinom Ackerman Metastase anaplastische Transformation verrucous carcinoma Ackerman metastasis anaplastic transformation 610 Medizin 33 Medizin XH 6700 ddc:610
8	Exploiting Drosophila as a model system for studying anaplastic lymphoma kinase in vivo Eriksson, Therese January 2010 (has links) Anaplastic Lymphoma Kinase (ALK) is a Receptor Tyrosine Kinase (RTK) and an oncogene associated with several human diseases, but its normal function in humans and other vertebrates is unclear. Drosophila melanogaster has an ALK homolog, demonstrating that the RTK has been conserved throughout evolution. This makes Drosophila a suitable model organism for studying not only Drosophila ALK function, but also to study mammalian forms of ALK. In Drosophila the ligand Jeb activates ALK, initiating signaling crucial for visceral mesoderm development. The activating ligand for mammalian ALK is unclear, and for this reason Drosophila was employed in a cross-species approach to investigate whether Drosophila Jeb can activate mouse ALK. Jeb is unable to activate mouse ALK, and therefore mouse ALK is unable to substitute for and rescue the Drosophila ALK mutant phenotype. This suggests that there has been significant evolution in the ALK-ligand relationship between the mouse and Drosophila. In humans ALK has recently been shown to be involved in the development of neuroblastoma, a cancer tumor in children. I have developed a Drosophila model for examining human gain of function ALK mutants found in neuroblastoma patients. The various ALK variants have acquired point mutations in the kinase domain that have been predicted to activate the RTK in a constitutive and ligand independent manner. When expressed in the fly eye, active human ALK mutants result in a rough eye phenotype, while inactive wild type ALK does not, due to the lack of an activating ligand in the fly. In this way several of the ALK mutations identified in neuroblastoma patients could be confirmed to be activated in a ligand independent manner. Moreover, a novel ALK mutant; ALKF1174S, was discovered in a neuroblastoma patient and was in the Drosophila model shown to be a gain of function mutation, and a previously predicted gain of function mutation; ALKI1250T, was shown to be a kinase dead mutation. This fly model can also be used for testing ALK selective inhibitors, for identifying activating ligands for human ALK and for identifying conserved components of the ALK signaling pathway. Gut musculature development in Drosophila is dependent on ALK signaling, while somatic muscle development is not. Proteins of the Wasp-Scar signaling network regulate Arp2/3-complex mediated actin polymerization, and I have investigated their function in visceral and somatic muscle fusion. I found that Verprolin and other members of this protein family are essential for somatic but not visceral muscle development. Despite fusion defects in both tissues in Verprolin and other examined mutants, gut development proceeds, suggesting that fusion is not crucial for visceral mesoderm development. Hence the actin polymerization machinery functions in both somatic and visceral muscle fusion, but this process only appears to be essential in somatic muscle development. / Exploiting Drosophila as a model system for studying Anaplastic Lymphoma Kinase in vivo Anaplastic lymphoma kinase Receptor tyrosine kinase Jeb neuroblastoma actin polymerization Wasp Scar Vrp1 Arp2/3 Molecular biology Molekylärbiologi
9	The Role of Online Support for Anaplastic Thyroid Cancer Patients and Survivors Nixon, Bevin J 01 January 2019 (has links) The rate of thyroid cancer diagnosis has risen, and researchers' findings point to improved diagnostic testing and overdiagnosis as well as increases in actual incidences as the reasons behind this rise. With improved treatments and testing methods, the number of thyroid cancer survivors has also increased. Thyroid cancer presents challenges to coping and can cause significant stress in an individual's life. More specifically, anaplastic thyroid cancer (ATC) creates complicated challenges for patients and survivors. The problem is patients need support during diagnosis and treatment when adjusting to their 'new normal' and may be reaching to Internet based social support groups to gain health information. Lazarus's transactional theory of stress and coping formed a framework for this generic qualitative exploration of the types of support and information ATC patients and survivors receive through participating in an online Facebook support group. Thematic content analysis was conducted on archival data collected from the group over 4 months, namely 2,384 posts created by 166 group members. From this analysis, a picture relevant to all group participants was developed to include themes found among the data. Themes of emotional, informational and spiritual support emerged as well as the significance of using emojis as symbolic expressions of support. Implications for social change include expanding the theoretical knowledge of the ATC patient and survivor experience and the types of support available in online environments. This knowledge can lead to positive social change in terms of improving support resources, which may help in recovery from ATC; lessening the burden on patients, families, providers, insurance, the healthcare system, and our society as a whole. Anaplastic thyroid cancer online support social support support group thyroid cancer Communication Technology and New Media Medicine and Health Sciences Social Work
10	Klinischer Verlauf und Analyse des Rezidivmusters von 111 Patienten mit anaplastischem Astrozytom oder Glioblastoma multiforme nach Operation und lokaler Strahlentherapie Graubner, Sebastian 25 May 2005 (has links) Die vorliegende Arbeit ist eine retrospektive Kohortenstudie, welche alle Patienten einschloß, die im Zeitraum von 07/1988 bis 06/1997 aufgrund eines anaplastischen Astrozytoms oder eines Glioblastoma multiforme im damaligen Rudolf-Virchow-Klinikum in Berlin eine Strahlentherapie des Kopfes erhielten. Von den 111 Patienten erlitten im Beobachtungszeitraum 85 ein radiologisches Rezidiv. Die mediane Überlebenszeit betrug 9 Monate. 69 der Rezidive waren Zentralrezidive, 7 Randrezidive und 9 Fernrezidive. Auch die Rand- und Fernrezidive rezidivierten zusätzlich am Ort der Primärläsion. Es konnte gezeigt werden dass ein Sicherheitsabstand von 2-3 cm ausreicht um 90% der Rezidive vollständig zu erfassen und dass die lokale Kontrolle weiterhin das Hauptproblem bei der Behandlung dieser malignen Gliome ist. / This retrospective study reviews the data of 111 patients treated from 07/1988 to 06/1997 at the Rudolf-Virchow-Klinikum in Berlin. Both patients with anaplastic astrocytoma and glioblastoma multiforme were included. 85 patients showed radiological recurrence of tumour. Median survival was 9 months. 69 recurrences were central, 7 near and 9 distant recurrences. Near and distant recurrences were always multifocal, i. e. they recurred also at central locations. It was shown that a safety margin of 2-3 cm is sufficient to completely cover 90% of recurrent tumour. Local failure is still the primary difficulty in treating these malignant glioma. Glioblastoma multiforme Anaplastische Astrozytome maligne Gliome Rezidivanalyse anaplastic astrocytoma glioblastoma multiforme malignant glioma recurrence analysis 610 Medizin 33 Medizin XH 8554 XH 8578 YR 3128 ddc:610

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