Novel Approaches for the Molecular Targeting of Ewing's Sarcoma Family of Tumors |
An ESUN Article
Introduction
Current therapy for Ewing's Sarcoma Family of Tumors (ESFT) combines high-dose chemotherapy for systemic control of disease, with surgical and/or radiation therapeutic approaches for localized tumor control. Despite this multimodal treatment strategy the cure rate for localized disease is only 70%, and the cure rate for patients showing metastatic disease at presentation is less than 30%.
Background References
For more general information about the ESFT see "Ewing's Sarcoma Family of Tumors (ESFT)" by R. Lor Randall, MD, Vol. 1, No. 3 ESUN 2005.
For general information on medical or biological terms and biological principles see:
Help Me Understand Genetics Handbook on the Genetics Home Reference website (the handbook gcan be reaf online of downloaded in its entirety).
DNA-RNA-Protein Introduction on the Nobelprize.com website (make sure to click on the link, "Learn how to navigate in the document").
The Medical Dictionary hosted on the MedlinePlus website.
The National Institute of General Medical Sciences pamphlet, Inside the Cell, provides a useful and easily understood introduction to cells. The pamphlet can either be read on-line or downloaded as an Acrobat PDF document).
Many new pharmaceutical agents have been tested in early phases of clinical trials in ESFT patients who have recurrent disease. While some agents led to partial response or stable disease, the percentage of drugs eliciting responses or causing an overall effect have been minimal. The most promising new chemotherapeutics resulting from phase II clinical trials, seem to be topotecan and its derivative irinotecan [1], [2], and [3]. During the last couple of years, small numbers of ESFT patients have been treated with docetaxel [4], gemcitabine [5], bortezomib [6] or ecteinascidin-743 [7] in phase I and II trials with no significant improvement to disease cure or stabilization. Furthermore, of the new pharmaceuticals being introduced to clinical practice, the most effective agents also have dose-limiting toxicities. Novel approaches to minimize non-specific toxicity are needed both for patients with recurrence and at diagnosis.
Typically, ESFT contains a cytogenetic abnormality−a chromosomal translocation between the EWS gene (chromosome 22) and one of the genes FLI1, ERG, ETV1 or FEV. In the vast majority of cases this leads to the expression of the EWS-FLI1 (EF) chimeric fusion protein (see Figures 1-3).
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A chromosomal translocation is the exchange of fragments between two (or more) chromosomes during cell division. If the breakpoint occurs within two genes the joint of these chromosomal parts may result in a fusion gene giving rise to a functional, but aberrant protein.
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EF expression is necessary for tumorigenesis in ESFT cells [8] and elimination of EF in laboratory models leads to ESFT cell death [9-11]. While ESFT cells appear to require EF for growth the non-rearranged EWS gene seems dispensable [12]. EF is not expressed in any cells except those of ESFT. Therefore, EF targeting would, in theory, only affect ESFT cells. Despite this specific tumor target there is no treatment available that directly targets EF. However, ESFT research in recent years has been characterized by the development of some encouraging new strategies that reduce the expression or function of EF. Some of the most promising approaches are going to be discussed in the following paragraphs.
1. Inhibitory oligonucleotides
The most direct specific approach to inactivate EF is based on short nucleotide sequences (called oligonucleotides) which can pair with the single stranded mRNA molecule which codes for the EF protein sequence. These oligonucleotides hybridize to specifically selected sequences and thereby halt protein translation and mRNA splicing. Subsequently, EF protein levels are significantly reduced. There are two slightly different biological methods to achieve this goal.
a. Antisense technology: Antisense oligonucleotides are short, synthetic single stranded DNA molecules that are complimentary, or antisense, to a specific target sequence on the RNA. Hybridization of these antisense oligonucleotides to their target sequence in the cells results in degradation of the mRNA, thereby preventing the generation of a functional protein. In laboratory cell line models antisense oligonucleotides are easy to administer. In general they need to be chemically modified to block their degradation. Cumulative clinical and preclinical data suggest that antisense technology has the potential to result in new treatment strategies for a variety of diseases. The first antisense drug (Viltravene™ from Isis/Novartis) recently received FDA approval for treatment of cytomegalovirus (CMV) retinitis in AIDS patients. This treatment is largely successful because the drug is administered by injection directly into the eye, a procedure not readily translatable to ESFT patients.
b. siRNA: The second mechanism used to block RNA translation is called siRNA (inhibitory RNAs) which are short double stranded RNAs of approximately 19-21 base pairs in length. Similar to antisense oligonucleotides their sequence is specifically selected to match a particular target sequence (e.g. EF). To efficiently pair one strand of these inhibitory RNAs to the transcript and to subsequently destroy the transcript, a different set of enzymes (dicers) must be activated.
For several reasons inhibitory oligonucleotides never yield a complete absence of the targeted protein. In addition, while theses strategies are being actively investigated, their delivery to human tumors currently proposes a technical challenge. Therefore antisense/siRNA strategies may not provide an additional benefit at this time, but suggest promise in the future.
2. Antibodies
Antibodies are protein molecules that the immune system uses to target so called antigens. Antibodies can be directed to extracellular surface antigens and also to intracellular antigens. For the intracellular application they have to be delivered by similar methods as inhibitory oligonucleotides, which allow them to penetrate the cell membrane. This alternative approach to inhibitory oligonucleotides employs specific recombinant antibodies (so called single chain antibodies) to inhibit EF function. Their key advantage is the ability to genetically engineer those antibodies in a way that intracellularly directs them to the target proteins place of action.
Genetic engineering of an antibody alters its protein sequence using molecular-biological methods to increase its efficacy of binding to its target or to direct the antibody to special intracellular compartments like the nucleus.
It was recently reported, that recombinant antibody technology was used to successfully interfere with wild type EWS protein [13]. Unfortunately the described antibody does not have any impact on the EF chimeric protein. This may, in part, be a result of the originally performed screening strategy and the difficulty in obtaining structurally unaltered and functionally active native EF. However, single-chain antibodies are a theoretically promising strategy, worthy of further investigation.
ESFT uses critical signaling surface proteins that might result in antibody-targeted therapy. The IGF pathway [14] has been inhibited with antibodies and in combination with chemotherapy might lead to therapeutic advances. IGF-IR antibodies are also undergoing current clinical development and are likely to be tested in upcoming ESFT trials. ESFT express the CD99 antigen on their external cell membrane, but the function of CD99 is cryptic. Antibodies directed towards the ESFT surface marker CD99, along with doxorubicin based chemotherapy [15] achieved a delay in tumor growth and improved survival in animal models.
3. Disrupting protein interactions
Inhibiting the EF protein function is the main goal of our laboratory. Transcription factors, like EF, function in a large multiprotein transcriptional complex. Therefore, EF, like other transcription factors relies on direct protein-protein interaction. We recently discovered EF interacts with RNA helicase A (RHA), an RNA/DNA unwinding enzyme involved in many basic cellular functions like replication, transcription and translation [16]. Our work studying the interaction of RHA with EF suggests that RHA is necessary for EF tumorigenic function. We have begun to develop strategies to prevent RHA from interacting with EF as a mechanism to inhibit the growth of ESFT. One possible way to disrupt this binding is to use a short protein sequence (called a peptide) that mimics the specific RHA region that binds to EF. This peptide competes with the wild type RHA for the binding site on EF, thereby inactivating the functional transcription complex. Our current research is directed towards interrupting the interaction between EF and its protein partners with small molecules specifically designed to mimic certain functionally active protein domains. Like a peptide mimic, these drugs would keep EF apart from its interacting proteins. The small molecules can be modified to have properties that would allow them to become clinically useful pharmaceuticals, including avoiding degradation in the serum and penetrating the cell membrane.
4. Novel immune approaches
Alternatively, antitumor therapies may also be combined with immune modulating therapies.
Immune-modulation is the process of influencing the immune system to suppress its disadvantageous effects or to stimulate wanted ones.
Intratumoral transfer of the IL-12 gene results in a suppression of local and distant Ewing’s sarcoma in murine tumor models [17]. Unfortunately these kinds of gene therapy, although tested in clinical trials for a variety of diseases, have not become clinically validated. Tumor-specific EF based peptide vaccinations are supposed to increase a patients’ immune defense against tumor cells, but pilot studies made with translocation specific protein fragments did not alter the clinical outcome for ESFT patients [18].
Peptide vaccination: Disease specific immunogens can usually be reduced to small fragments of a protein (peptides). Also, in case of cancer. The sequence of these peptides can be determined and they can subsequently be produced synthetically in larger amounts. As immunization with common vaccines lead to immunity to a variety of other diseases, vaccination with cancer specific peptides is hoped to induce an antitumor response.
Gene therapy is the insertion or replacement of absent or mutated genes into an individuals cells or tissue to treat genetic disorders. It thereby fixes the problem at its roots. Gene therapy is also used to insert genes in tumor cells to endogenously produce proteins which support or elicit an immune response to this tumor.
The Tissues of the Human Body: An Introduction is designed to acquaint you with the basic characteristics of tissues, including soft tissues. The design of this website, allows you to step "through tissue categories and topics to learn key characteristics of each tissue type."
The EWS-FLI1 protein in ESFTs is a potential therapeutic target, that is critical for ESFT survival and only present in ESFT cells. The challenge is how to harness this unique target and create specific therapies. Knowledge of how EF functions continues to accrue and this knowledge will lead to novel ways that specifically and effectively treat patients. The parallel increase in technology, such as delivery systems, will likewise benefit future patients. Patients with ESFT will benefit from ongoing investigations that will hopefully allow for more successful and less toxic therapies.
References
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V4N3 ESUN Copyright © 2007 Liddy Shriver Sarcoma Initiative.