Targeted therapies in cancer - challenges and chances offered by newly developed techniques for protein analysis in clinical tissues

Malinowsky, Katharina; Wolff, Claudia; Gündisch, Sibylle; Berg, Daniela; Becker, Karl‐Friedrich

doi:10.7150/jca.2.26

Cited by 21 publications

(15 citation statements)

References 78 publications

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“…Therefore p16 INK4a is used as an HPV-related surrogate marker in many study protocols because the procedure is well-established and time saving [20, 21]. It has a distinct role in cell cycle regulation [22], acting as a tumour suppressor protein. It is well known that detection of HPV infection with p16 INK4a staining often does not give accurate results [23, 24].…”

Section: Introductionmentioning

confidence: 99%

Impact of HPV infection on oral squamous cell carcinoma

et al. 2016

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BackgroundHead and neck squamous cell carcinomas (HNSCC) are often divided by their aetiology. Noxae associated collectives are compared with the human papilloma virus (HPV)-associated group, whereas different localisations of oral (OSCC) and oropharyngeal (OPSCC) squamous cell carcinomas are mostly discussed as one single group. Our aim was to show that classification by aetiology is not appropriate for OSCC.ResultsHPV DNA was detected by PCR in 7 (3.47%) patients, and we identified 12 (5.94%) positive (+) cases by p16INK4a immunostaining. Only 4 (1.98%) of the p16INK4a+ cases were + for HPV using PCR. Our homogenous collective of OSCC allowed us to compare HPV+ and HPV negative (−) patients without creating bias for tumour localisation, age, gender or tumour stage.Materials and methodsAfter testing OSCC samples for HPV positivity, we compared the results of two commonly used HPV detection methods, p16INK4a immunostaining and HPV DNA-related PCR, on 202 OSCC patients. HPV subtypes were determined with an HPV LCD Array Kit. Clinicopathological features of the patients were analysed, and the disease specific survival rates (DSS) for HPV+ and HPV− patients were obtained.Conclusionsp16INK4a immunostaining is a not a reliable HPV detection method for OSCC. Positive p16INK4a immunostaining did not agree with + results from PCR of HPV DNA. Furthermore, the influence of HPV-related oncogenic transformation in OSCC is overestimated. The significance of HPV infection remains clinically unclear, and its influence on survival rates is not relevant to OSCC cases.

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Section: Introductionmentioning

confidence: 99%

Impact of HPV infection on oral squamous cell carcinoma

et al. 2016

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“…[1][2][3]38,39 Antibodies have assumed an important role in targeted therapy over the past several years. Customized cell lines are developed to engineer antibodies that recognize a specific target.…”

Section: Two Types Of Targeted Therapiesmentioning

confidence: 99%

The Journey Toward Personalized Cancer Therapy

Tulbah¹,

Chaudhri

Dayel³

et al. 2014

Advances in Anatomic Pathology

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Human cancer has been one of the most difficult and tenacious problems that has defied many therapeutic regimens in the past. In recent years, there has been an explosive growth in our knowledge about molecular cell biology of cancer leading to the development of several molecularly targeted therapies. These therapeutic agents are used specifically for those tumors that are found to be susceptible to such a therapeutic approach. These therapies include a variety of monoclonal antibodies that target cell-surface receptors or, in some cases, their ligands. A second type of targeted therapies consists of small molecules that are designed to inhibit tyrosine kinase activity within the cancer cells. Despite initial optimism, this approach to cancer therapy is proven to be problematic because of inherent cancer heterogeneity and frequent development of drug resistance. The targeted therapies have improved survival time for many cancer patients but have not provided any definitive cures. The treating physicians constantly face the daunting challenge of balancing expected benefit with risk for complications, to achieve the most successful outcome. Still, the results often fall short of expectations. Personalized cancer treatment on the basis of targeted therapies is certainly an achievable goal, but more work is needed to make it a reality.

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“…[8] Likewise, challenges remain with respect to delivery to specific sites, real time tracking of the system and control over the release system after the drug has been transported to the target site. [9] In the present contribution, we formulated a module using super paramagnetic iron oxide nanoparticles (SPION) as the core, stabilised with stimuli-responsive hydrazide-terminated poly(styrene)-b-poly(acrylic acid) block copolymer (PS-b-PAA) as the shell, which was loaded with the anticancer drug, doxorubicin (DOx) and with peripheral surfacing by folic acid. The covalent linkage of folate served to recognise the cancer site and the pH-sensitive DOx bonds delivered effective release of the drug at the tumour site.…”

Section: Introductionmentioning

confidence: 99%

MRI‐Visual Order–Disorder Micellar Nanostructures for Smart Cancer Theranostics

Khaliq

Romu

Wiecheć

et al. 2013

Adv Healthcare Materials

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This development of MRI-visual order-disorder structures for cancer nanomedicine explores pH-trigger mechanism for theragnosis of tumour hallmark functions. Superparamagnetic iron oxide nanoparticles (SPIONs) stabilised with amphiphilic poly(styrene)-b-poly(acrylic acid)-doxorubicin with folic acid (FA) surfacing is employed as a multi-functional approach to specifically target, diagnose and deliver drugs via a single nanoscopic platform for cancer therapy. The functional aspects of the micellar nanocomposite is investigated in vitro using human breast SkBr3 and colon cancer HCT116 cell lines for the delivery, release, localisation and anticancer activity of the drug. Our work shows, for the first time, concentration dependent T 2 -weighted MRI contrast for a monolayer of clustered cancer cells. The pH tunable order-disorder transition of the core-shell structure induces the relative changes in MRI contrast. The outcomes elucidate the potential of this material for smart cancer theranostics by delivering non-invasive real-time diagnosis, targeted therapy and monitoring the course and response of the action before, during and after the treatment regimen.Submitted to 3

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Targeted therapies in cancer - challenges and chances offered by newly developed techniques for protein analysis in clinical tissues

Cited by 21 publications

References 78 publications

Impact of HPV infection on oral squamous cell carcinoma

Impact of HPV infection on oral squamous cell carcinoma

The Journey Toward Personalized Cancer Therapy

MRI‐Visual Order–Disorder Micellar Nanostructures for Smart Cancer Theranostics

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