Your search keyword '"Allegrini, Peter R."' showing total 7 results

1. Dual-Modal Magnetic Resonance/Fluorescent Zinc Probes for Pancreatic β-Cell Mass Imaging.

Author

Stasiuk, Graeme J., Sae-Heng, Myra, Rivas, Charlotte, Long, Nicholas J., Minuzzi, Florencia, Rutter, Guy A., Juretschke, Hans-Paul, Piemonti, Lorenzo, Allegrini, Peter R., Laurent, Didier, Duckworth, Andrew R., and Beeby, Andrew

Subjects

ZINC ions, BINDING sites, PANCREATIC beta cells, TRANSITION metal chelates, MAGNETIC resonance imaging, FLUORESCENCE

Abstract

Despite the contribution of changes in pancreatic β-cell mass to the development of all forms of diabetes mellitus, few robust approaches currently exist to monitor these changes prospectively in vivo. Although magnetic-resonance imaging (MRI) provides a potentially useful technique, targeting MRI-active probes to the β cell has proved challenging. Zinc ions are highly concentrated in the secretory granule, but they are relatively less abundant in the exocrine pancreas and in other tissues. We have therefore developed functional dual-modal probes based on transition-metal chelates capable of binding zinc. The first of these, Gd ⋅1, binds ZnII directly by means of an amidoquinoline moiety (AQA), thus causing a large ratiometric Stokes shift in the fluorescence from λem=410 to 500 nm with an increase in relaxivity from r1=4.2 up to 4.9 m M−1 s−1. The probe is efficiently accumulated into secretory granules in β-cell-derived lines and isolated islets, but more poorly by non-endocrine cells, and leads to a reduction in T1 in human islets. In vivo murine studies of Gd ⋅1 have shown accumulation of the probe in the pancreas with increased signal intensity over 140 minutes. [ABSTRACT FROM AUTHOR]

Published

2015

2. Quantitative dynamic contrast-enhanced MRI in tumor-bearing rats and mice with inversion recovery TrueFISP and two contrast agents at 4.7 T.

Author

Weidensteiner, Claudia, Rausch, Martin, McSheehy, Paul M.J., and Allegrini, Peter R.

Abstract

Purpose: To characterize tumor vascularization by dynamic-contrast enhanced (DCE) MRI using low and medium molecular weight paramagnetic contrast agents (CA) and inversion recovery (IR) true fast imaging with steady state precession (TrueFISP) in tumor-bearing rats and mice.Materials and Methods: T(1) mapping was performed using IR True FISP in phantoms and in vivo at 4.7 T and validated with a segmented IR gradient-echo (IR GE) method. CA concentration in DCE-MRI studies in vivo was calculated from time-series T(1) maps using the CAs GdDOTA and P792 (low and medium molecular weight, respectively). Standard vascular input functions (VIFs) were measured in the jugular veins and were used for modeling of the CA kinetics with a two-compartment model. In rat breast tumors, vascular permeability (transfer constant K(trans)), fractional plasma volume v(p), and fractional leakage space v(e) were quantified and parametric maps were generated.Results: The IR TrueFISP T(1) was slightly underestimated in phantoms and overestimated in vivo (10%) with respect to IR GE. VIFs showed only small interindividual variation. Mean K(trans) values were 0.062 +/- 0.017 min(-1) for GdDOTA and 0.015 +/- 0.005 min(-1) for P792 (N = 12). Mean v(e) and v(p) values were 0.15 +/- 0.04 (0.09 +/- 0.03) and 0.04 +/- 0.01 (0.03 +/- 0.01) for GdDOTA (P792).Conclusion: DCE-MRI with IR TrueFISP provided absolute values for K(trans), v(p), and v(e). Direct comparison between GdDOTA and P792 revealed significant differences in the VIF, model-fit-quality, permeability, leakage space, and plasma volume. The larger molecular weight CA P792 appears to be better for measuring tumor vascular parameters. [ABSTRACT FROM AUTHOR]

Published

2006

3. PTK787/ZK222584, a tyrosine kinase inhibitor of vascular endothelial growth factor receptor, reduces uptake of the contrast agent GdDOTA by murine orthotopic B16/BL6 melanoma tumours and inhibits their growth in vivo.

Author

Rudin, Markus, McSheehy, Paul M. J., Allegrini, Peter R., Rausch, Martin, Baumann, Diana, Becquet, Mike, Brecht, Karin, Brueggen, Josef, Ferretti, Stephane, Schaeffer, Fabienne, Schnell, Christian, and Wood, Jeanette

Abstract

Assessment of tumour vascularity may characterize malignancy as well as predict responsiveness to anti-angiogenic therapy. Non-invasive measurement of tumour perfusion and blood vessel permeability assessed as the transfer constant, Ktrans, can be provided by dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI). Using the orthotopic murine tumour model B16/BL6 melanoma, the small contrast agent GdDOTA (DOTAREM®; Guerbet, Paris) was applied to assess the vascular transfer constant, Ktrans, and interstitial leakage space, whereas intravascular iron oxide nanoparticles (Endorem®; Guerbet, Paris) were used to detect relative tumour blood volume (rTBV), and in one experiment blood flow index (BFI). No correlations were observed between these four parameters ( r2 always <0.05). The B16/BL6 primary tumour and lymph-node cervical (neck) metastases produced high levels of the permeability/growth factor, VEGF. To probe the model, the novel VEGF receptor (VEGF-R) tyrosine kinase inhibitor, PTK787/ZK222584 (PTK/ZK) was tested for anti-tumour efficacy and its effects on DCE-MRI measured parameters of tumour vascularity. Data from the non-invasive measure of tumour vascularity were compared with a histological measurement of vasculature using the DNA-staining dye H33342. PTK/ZK inhibited growth of the primary and, particularly, cervical tumour metastases following chronic treatment for 2 weeks (50 or 100 mg/kg daily) of 1-week-old tumours, or with 1 week of treatment against more established (2-week-old) tumours. After chronic treatment with PTK/ZK, DCE-MRI detected significant decreases in Ktrans and interstitial leakage space, but not rTBV of both primary tumours and cervical metastases. Histological data at this time-point showed a significant decrease in blood vessel density of the cervical metastases but not the primary tumours. However, in the cervical metastases, the mean blood vessel width was increased by 38%, suggesting overall no marked change in blood volume. After acute (2-4 day) treatment, DCE-MRI of the cervical metastases demonstrated a significant decrease in Ktrans and interstitial leakage space and also in the initial area under the enhancement curve for GdDOTA (IAUC), but no change in the rTBV or BFI. Thus, significant changes could be detected in the DCE-MRI measurement of tumour uptake of a small contrast agent prior to changes in tumour size, which suggests that DCE-MRI could be applied in the clinic as a rapid and sensitive biomarker for the effects of VEGF-R inhibition on tumour blood vessel permeability and thus may provide an early marker for eventual tumour response. Copyright © 2005 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2005

4. Thrombolysis induces cerebral hemorrhage in a mouse model of cerebral amyloid angiopathy.

Author

Winkler, David T., Biedermann, Luc, Tolnay, Markus, Allegrini, Peter R., Staufenbiel, Matthias, Wiessner, Christoph, and Jucker, Mathias

Published

2002

5. Long-term protection of brain tissue from cerebral ischemia by peripherally administered peptidomimetic caspase inhibitors.

Author

Deckwerth, Thomas L., Adams, Lisa M., Wiessner, Christoph, Allegrini, Peter R., Rudin, Markus, Sauter, Andre, Hengerer, Bastian, Sayers, Robert O., Rovelli, Giorgio, Aja, Teresa, May, Rachel, Nalley, Kip, Linton, Steve, Karanewsky, Donald S., Wu, Joe C., Roggo, Silvio, Schmitz, Albert, Contreras, Patricia C., and Tomaselli, Kevin J.

Published

2001

6. Combined blockade of endothelin-1 and thromboxane A2 receptors against postischaemic contractile dysfunction in rat hearts.

Author

Hornstein, Pius S, Zaugg, Christian E, Zhu, Peili, Allegrini, Peter R, and Buser, Peter T

Published

2001

7. Differentiation of proliferating from resting cartilage in human fetal nasal septum by magnetic resonance imaging.

Author

Allegrini, Peter R., van Velzen, Dick, van Loosen, John, and Bullock, Gillian R.

Published

1990