2005
DOI: 10.2174/138161205774414556
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Direct Evidence on the Immune-Mediated Spontaneous Regression of Human Cancer: An Incentive for Pharmaceutical Companies to Develop a Novel Anti-Cancer Vaccine

Abstract: To develop an effective pharmaceutical treatment for a disease, we need to fully understand the biological behavior of that disease, especially when dealing with cancer. The current available treatment for cancer may help in lessening the burden of the disease or, on certain occasions, in increasing the survival of the patient. However, a total eradication of cancer remains the researchers' hope. Some of the discoveries in the field of medicine relied on observations of natural events. Among these events is th… Show more

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Cited by 24 publications
(15 citation statements)
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“…These conclusions drawn from animal models are very likely to apply to cancer patients as well. It is true however, that some cancers spontaneously regress with signs of immune responses [25]. These latter cancers can be viewed as equivalent to the ''good'' tumors described in the experimental models above, but they are unfortunately not the only type.…”
mentioning
confidence: 99%
“…These conclusions drawn from animal models are very likely to apply to cancer patients as well. It is true however, that some cancers spontaneously regress with signs of immune responses [25]. These latter cancers can be viewed as equivalent to the ''good'' tumors described in the experimental models above, but they are unfortunately not the only type.…”
mentioning
confidence: 99%
“…This is largely due to the rapid identification of tumour-associated antigens (TAAs), which has been achieved by examining the specificity of existing T-cell responses (Stevanovic, 2002), or by using screening strategies such as serological identification of antigens by recombinant expression cloning (SEREX) (Pfreundschuh, 2000), proteomic analysis, gene expression profiling or combinations (Schultze and Vonderheide, 2001). The first tumour-specific vaccination was carried out in malignant melanoma which remains a valuable model for investigating cancer immunotherapy in humans (Saleh et al, 2005). With the growing number of TAAs identified, clinical studies have been expanded to other carcinomas (Stevanovic, 2002) and most of these studies used MHC class I-restricted, T-cell epitope peptides derived from TAAs to expand cytotoxic T cells (CTLs) for tumour destruction.…”
mentioning
confidence: 99%
“…Das applizierte Therapieschema führte damit zum Ausschluss der Patienten mit guter Immunantwort, d.h. von denjenigen, die mit starker Lokalreaktion oder Fieber reagieren konnten. Möglicherweise sind damit Patienten mit guter Prognose ausgeschlossen [26] und weniger immunkompetente Patienten (mit schlechterer Prognose) selektioniert worden. Somit liegt der Verdacht auf eine dritte Verzerrung vor, hier durch Selektion innerhalb der Therapiegruppe gegenüber der Kontrolle.…”
Section: Analyse Der Ausgewählten Randomisierten Studie [12]unclassified