Podrobný výpis o publikaci

SVOBODA, Marek. Molecular taxonomy and predictive systems of human cancers based on gene expression profiling. In ANALYTICAL CYTOMETRY IV. BOOK OF ABSTRACTS. 1. vyd. Brno: Česká společnost pro analytickou cytologii, 2007, s. 80. ISBN 978-80-239-9591-6.

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TY  - JOUR
ID  - 726201
AU  - Svoboda, Marek
PY  - 2007
TI  - Molecular taxonomy and predictive systems of human cancers based on gene expression profiling.
PB  - Česká společnost pro analytickou cytologii
CY  - Brno
SN  - 9788023995916
KW  - molecular taxonomy;cancer;gene expression
N2  - The diagnosis of malignancies is currently based on morphology and analysis of a few molecular markers of cancer cells. On the other hand, responses to treatment and clinical outcomes of patients within existent diagnostic categories are heterogeneous. What is the reason of this situation? The inadequacy of existing diagnostic methods or existing diagnostic categories? The complete elucidation of the human genome and the development of microarray technology have heralded a new era for biological sciences and medicine, particularly in cancer (Lander, 2001). Cancer is, in essence, a genetic disease. The DNA microarray technology represents a tool capable of both, simultaneously detecting and quantifying expression of tens of thousands of genes (expression profiling) in a very short period of time (Svoboda, 2004), thus provide for us molecular portrait and new insights into the biological processes underlying complex diseases such as cancer. Therefore, DNA microarrays are used to identify new molecular markers important for diagnostic and classification of many human cancers and prediction of treatment outcome (Sorlie, 2003). The aim of this presentation is to briefly review the analyses of two model malignancies studied in recent years, to illustrate the contribution of microarray technology to "personalized medicine". I will focus on diffuse large B-cell lymphoma (DLBCL), as a model of hematological malignancies, and breast cancer, as a model of solid tumors. In both cases, microarrays studies revealed new unexpected subgroups of the disease (e.g. "Germinal Center B-cell like DLBCL" vs "Activated B-cell like DLBCL", and "Basal-like", "Luminal-like A" and "Luminal-like B" breast cancer), and this stratification was correlated with the response to therapy and patients survival. In both cases, the extrapolation of these findings to more timely efficient and cost-effective methods, such as immunohistochemistry, is recently implemented in successive steps into clinical practice (Svoboda, 2006a, Svoboda, 2006b).
ER  -

Základní údaje
Originální název	Molecular taxonomy and predictive systems of human cancers based on gene expression profiling.
Název česky	Molekulární taxonomie a prediktivní systémy lidských novotvarů založených na profilování genové exprese.
Autoři	SVOBODA, Marek.
Vydání	1. vyd. Brno, ANALYTICAL CYTOMETRY IV. BOOK OF ABSTRACTS. s. 80-80, 2007.
Nakladatel	Česká společnost pro analytickou cytologii

Další údaje
Originální jazyk	angličtina
Typ výsledku	Stať ve sborníku
Obor	30200 3.2 Clinical medicine
Stát vydavatele	Česká republika
Utajení	není předmětem státního či obchodního tajemství
Organizační jednotka	Lékařská fakulta
ISBN	978-80-239-9591-6
Klíčová slova anglicky	molecular taxonomy;cancer;gene expression
Štítky	cancer, GENE EXPRESSION, molecular taxonomy
Příznaky	Mezinárodní význam, Recenzováno
Změnil	Změnil: prof. MUDr. Marek Svoboda, Ph.D., učo 19402. Změněno: 17. 12. 2007 04:29.

Anotace
The diagnosis of malignancies is currently based on morphology and analysis of a few molecular markers of cancer cells. On the other hand, responses to treatment and clinical outcomes of patients within existent diagnostic categories are heterogeneous. What is the reason of this situation? The inadequacy of existing diagnostic methods or existing diagnostic categories? The complete elucidation of the human genome and the development of microarray technology have heralded a new era for biological sciences and medicine, particularly in cancer (Lander, 2001). Cancer is, in essence, a genetic disease. The DNA microarray technology represents a tool capable of both, simultaneously detecting and quantifying expression of tens of thousands of genes (expression profiling) in a very short period of time (Svoboda, 2004), thus provide for us molecular portrait and new insights into the biological processes underlying complex diseases such as cancer. Therefore, DNA microarrays are used to identify new molecular markers important for diagnostic and classification of many human cancers and prediction of treatment outcome (Sorlie, 2003). The aim of this presentation is to briefly review the analyses of two model malignancies studied in recent years, to illustrate the contribution of microarray technology to "personalized medicine". I will focus on diffuse large B-cell lymphoma (DLBCL), as a model of hematological malignancies, and breast cancer, as a model of solid tumors. In both cases, microarrays studies revealed new unexpected subgroups of the disease (e.g. "Germinal Center B-cell like DLBCL" vs "Activated B-cell like DLBCL", and "Basal-like", "Luminal-like A" and "Luminal-like B" breast cancer), and this stratification was correlated with the response to therapy and patients survival. In both cases, the extrapolation of these findings to more timely efficient and cost-effective methods, such as immunohistochemistry, is recently implemented in successive steps into clinical practice (Svoboda, 2006a, Svoboda, 2006b).

Anotace

The diagnosis of malignancies is currently based on morphology and analysis of a few molecular markers of cancer cells. On the other hand, responses to treatment and clinical outcomes of patients within existent diagnostic categories are heterogeneous. What is the reason of this situation? The inadequacy of existing diagnostic methods or existing diagnostic categories? The complete elucidation of the human genome and the development of microarray technology have heralded a new era for biological sciences and medicine, particularly in cancer (Lander, 2001). Cancer is, in essence, a genetic disease. The DNA microarray technology represents a tool capable of both, simultaneously detecting and quantifying expression of tens of thousands of genes (expression profiling) in a very short period of time (Svoboda, 2004), thus provide for us molecular portrait and new insights into the biological processes underlying complex diseases such as cancer. Therefore, DNA microarrays are used to identify new molecular markers important for diagnostic and classification of many human cancers and prediction of treatment outcome (Sorlie, 2003). The aim of this presentation is to briefly review the analyses of two model malignancies studied in recent years, to illustrate the contribution of microarray technology to "personalized medicine". I will focus on diffuse large B-cell lymphoma (DLBCL), as a model of hematological malignancies, and breast cancer, as a model of solid tumors. In both cases, microarrays studies revealed new unexpected subgroups of the disease (e.g. "Germinal Center B-cell like DLBCL" vs "Activated B-cell like DLBCL", and "Basal-like", "Luminal-like A" and "Luminal-like B" breast cancer), and this stratification was correlated with the response to therapy and patients survival. In both cases, the extrapolation of these findings to more timely efficient and cost-effective methods, such as immunohistochemistry, is recently implemented in successive steps into clinical practice (Svoboda, 2006a, Svoboda, 2006b).

Anotace česky
Publikace je pouze v anglickém jazyce.

Návaznosti
NR9076, projekt VaV	Název: Genomické profilování v predikci odpovědi na chemoradioterapii u pacientů s lokálně pokročilým karcinomem konečníku