In Vitro Selection of RNA Aptamers That Bind to Cell Adhesion Receptors of Trypanosoma cruzi and Inhibit Cell Invasion

Ulrich, Henning; Magdesian, Margaret H.; Alves, Maria Júlia M.; Colli, Walter

doi:10.1074/jbc.m111859200

Cited by 145 publications

(130 citation statements)

References 42 publications

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“…�s interesting examples, members of the Gp85/TS family are developmentally regulated by postranscriptional mechanisms, with Gp82 and Tc85 glycoproteins expressed mainly in the MT and TCT forms, respectively. Gp82 binds to gastric mucin and Tc85 binds to members of the laminin and fibronectin families in the extracellular matrix (ECM); however, other receptors cannot be ruled out as Tc85 molecules have been described as multi-adhesion glycoproteins (Wirth & Kierszenbaum 1984, Ouaissi et al 1984, 1985, Noisin & Villalta 1989, Santana et al 199�, Magdesian et al 2001, Ulrich et al 2002, Nde et al 200�, Yoshida 2008 (Magdesian et al 200�). On the other hand, it has been shown that an inactive form of TS from TCT that binds sialic acid triggers NF-kB activation, the expression of adhesion molecules on endothelial cells and upregulation of parasite entry in a FLY-independent and carbohydrate-dependent way (Dias et al 2008).…”

Section: Signalling Mechanisms and Molecules Involved In T Cruzi Invmentioning

confidence: 99%

A century of research: what have we learned about the interaction of Trypanosoma cruzi with host cells?

Alves

Mortara

2009

Mem. Inst. Oswaldo Cruz

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Section: Signalling Mechanisms and Molecules Involved In T Cruzi Invmentioning

confidence: 99%

A century of research: what have we learned about the interaction of Trypanosoma cruzi with host cells?

Alves

Mortara

2009

Mem. Inst. Oswaldo Cruz

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“…A whole series of aptamers that can bind protein targets inside and outside the cell can be found in the literature, which illustrates the potential of DNA or RNA aptamers as therapeutic modalities. Examples include aptamers to HIV related targets (Andreola et al, 2001;de Soultrait et al, 2002;Duzgunes 2001), hepatitis C (Biroccio et al, 2002;Hwang et al, 2000;Vo et al, 2003), Trypanosoma cruzi (Homann and Goringer, 1999;Homann and Goringer, 2001;Ulrich et al, 2002), prion proteins (Sayer et al, 2004;Weiss et al, 1997), thrombin (Bock et al, 1992;Griffin et al, 1993;Holland et al, 2000), anti-angiogenesis vascular endothelial growth factor (Blank et al, 2001;White et al, 2003), prostate specific membrane antigen (Lupold et al, 2002), among many others. Aptamers against the nucleolin are currently in clinical trials for the treatment of cancer with very promising results (www.antisoma.com).…”

Section: Aptamers As Therapeuticsmentioning

confidence: 99%

Aptamer-based therapeutics and their potential in radiopharmaceutical design

Ferreira

Missailidis

2007

Braz. arch. biol. technol.

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Aptamers, short, single stranded oligonucleotide entities, have been developed in the past 15 years against a plethora of targets and for a variety of applications. These range from inhibition of receptors and enzymes to the identification of small molecules in sensor applications, and from the development of targeted therapeutic to the design of novel diagnostic and imaging agents. Furthermore, aptamers have been designed for targets that cover a wide range of diseases, from HIV to tropical diseases, cancer and inflammation. Their easy development and flexibility of use and manipulation, offers further potential. In this paper we review their selection and consider some of the recent applications of aptamers in the design of radiopharmaceuticals for the targeted radiotherapy and medical imaging of disease.

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“…The SELEX technique has been used to isolate high affinity aptamers for a wide range of targets, including small organic molecules (13,14), peptides (15,16), soluble proteins such as growth factors, neuropeptides, (17)(18)(19)(20)(21)(22), cell surface epitopes (23), proteins exposed in their membrane environment (24), red blood cell membranes (25), and whole organisms such as parasites (26,27) and anthrax spores (28). Aptamers with possible future therapeutic importance include aptamers that target pathogens such as the hepatitis C virus (29), the HIV virus (30,31), and African and American trypanosomes (26,27).…”

Section: The Selex Techniquementioning

confidence: 99%

“…Aptamers with possible future therapeutic importance include aptamers that target pathogens such as the hepatitis C virus (29), the HIV virus (30,31), and African and American trypanosomes (26,27). Aptamers have also been shown to effectively block growth factor induced receptor activation.…”

Section: The Selex Techniquementioning

confidence: 99%

“…In many cases, the binding site of the antagonists or agonists used for the elution of high-affinity aptamers has not been determined. In other cases, the receptor for the antagonists or agonists used for displacement of the aptamer during the SELEX process is not even known, like for RNA aptamers competing with host-cell matrix molecules for their binding sites on unknown cell surface receptors of Trypanosoma cruzi (27). Larry Gold (one of the authors in Morris et al (25)) evolved aptamers against erythrocyte membranes that bind specifically to prior unidentified target proteins.…”

Section: Target Purification and Identificationmentioning

confidence: 99%

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RNA and DNA aptamers in cytomics analysis

2004

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BackgroundThe systematic evolution of ligands by exponential enrichment (SELEX) technique is a combinatorial library approach in which DNA or RNA molecules (aptamers) are selected by their ability to bind their protein targets with high affinity and specificity, comparable to that of monoclonal antibodies. In contrast to antibodies conventionally selected in animals, aptamers are generated by an in vitro selection process, and can be directed against almost every target, including antigens like toxins or nonimmunogenic targets, against which conventional antibodies cannot be raised.MethodsAptamers are ideal candidates for cytomics, as they can be attached to fluorescent reporters or nanoparticles in order to study biological function by fluorescence microscopy, by flow cytometry, or to quantify the concentration of their target in biological fluids or cells using ELISA, RIA, and Western blot assays.ResultsWe demonstrate the in vitro selection of anti‐kinin B1 receptor aptamers that could be used to determine B1 receptor expression during inflammation processes. These aptamers specifically recognize their target in a Northern‐Western blot assay, and bind to their target protein whenever they are exposed in the membrane.ConclusionsCurrently, aptamers are linked to fluorescent reporters. We discuss here the present status and future directions concerning the use of the SELEX technique in cytomics. © 2004 Wiley‐Liss, Inc.

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In Vitro Selection of RNA Aptamers That Bind to Cell Adhesion Receptors of Trypanosoma cruzi and Inhibit Cell Invasion

Cited by 145 publications

References 42 publications

A century of research: what have we learned about the interaction of Trypanosoma cruzi with host cells?

A century of research: what have we learned about the interaction of Trypanosoma cruzi with host cells?

Aptamer-based therapeutics and their potential in radiopharmaceutical design

RNA and DNA aptamers in cytomics analysis

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