Brain Tumor Pathology: Current Diagnostic Hotspots and Pitfalls -  Davide Schiffer

Brain Tumor Pathology: Current Diagnostic Hotspots and Pitfalls (eBook)

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2006 | 2006
VI, 272 Seiten
Springer Netherlands (Verlag)
978-1-4020-3998-0 (ISBN)
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Since Bailey and Cushing (1926), all brain tumor classifications have been called histogenetic. The nosographic position that the tumor types progressively acquired in the classification systems derived from the resemblance of tumor cells to those of the cytogenesis, modified whenever new information became available from different biological research fields and especially from molecular genetics. Classically, on the basis of the rough correspondence between the mature/immature aspect of tumor cells and the benign/malignant biological behavior of the tumors, the histological labels contained a prognostic significance. The supposed origin of the tumors was thus a factor for prognosis. Later on, with the concept of anaplasia (Cox, 1933; Kernohan et al., 1949) new criteria were introduced for establishing the malignancy grades of tumors. Immunohistochemistry and later molecular genetics further refined the prognostic diagnoses, substantially increasing the opportunities to recognize the cell origin of tumors, beside revealing the pathogenetic mechanisms. Prognoses became more accurate, as required by the greater and more targeted possibilities of therapy.
Since Bailey and Cushing (1926), all brain tumor classifications have been called histogenetic. The nosographic position that the tumor types progressively acquired in the classification systems derived from the resemblance of tumor cells to those of the cytogenesis, modified whenever new information became available from different biological research fields and especially from molecular genetics. Classically, on the basis of the rough correspondence between the mature/immature aspect of tumor cells and the benign/malignant biological behavior of the tumors, the histological labels contained a prognostic significance. The supposed origin of the tumors was thus a factor for prognosis. Later on, with the concept of anaplasia (Cox, 1933; Kernohan et al., 1949) new criteria were introduced for establishing the malignancy grades of tumors. Immunohistochemistry and later molecular genetics further refined the prognostic diagnoses, substantially increasing the opportunities to recognize the cell origin of tumors, beside revealing the pathogenetic mechanisms. Prognoses became more accurate, as required by the greater and more targeted possibilities of therapy.

Introduction Chapter 1: The origin of gliomas in relation with the histological diagnosis Chapter 2: Molecular genetics outline of brain tumors Chapter 3: General remarks Chapter 4: Astrocytic Tumors I Chapter 5: Astrocytic Tumors II Chapter 6: Oligodendroglian Tumors Chapter 7: Ependymal Tumors Chapter 8: Neuronal and /Mixed Glio-neural Tumors I Chapter 9: Neuronal and /Mixed Glio-neural Tumors II Chapter 10: Peculiar Tumors Chapter 11: Cell Migration and Invasion Chapter 12: Apoptosis Chapter 13: The Ubiquitin-proteasome System Chapter 14: Angiogenesis Chapter 15: Meningiomas

Erscheint lt. Verlag 28.7.2006
Zusatzinfo VI, 272 p.
Verlagsort Dordrecht
Sprache englisch
Themenwelt Medizin / Pharmazie Allgemeines / Lexika
Medizin / Pharmazie Medizinische Fachgebiete Chirurgie
Medizin / Pharmazie Medizinische Fachgebiete Neurologie
Medizin / Pharmazie Medizinische Fachgebiete Onkologie
Medizin / Pharmazie Studium
Schlagworte angiogenesis • Apoptosis • biopsy • Diagnostics • Glioma
ISBN-10 1-4020-3998-0 / 1402039980
ISBN-13 978-1-4020-3998-0 / 9781402039980
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