Literature DB >> 32172799

225Ac- and 213Bi-Substance P Analogues for Glioma Therapy.

Leszek Królicki1, Jolanta Kunikowska2, Frank Bruchertseifer3, Henryk Koziara4, Bartosz Królicki4, Maciej Jakuciński5, Dariusz Pawlak6, Rafał Rola7, Alfred Morgenstern3, Elżbieta Rosiak2, Adrian Merlo8.   

Abstract

Within the last decades, there has been no major improvement in treatment of patients with glioma, especially with glioblastoma multiforme (GBM) which is related to specific features of this tumor type, such as heterogeneity at the macroscopic, microscopic and genetic level, the infiltrative nature of tumors and the obstacle of the brain-blood barrier which limits the accessability of most drugs. The current standard of care is surgical resection, followed by radio- and chemotherapy. After first-line treatment of the primary lesion, tumor recurrence is diagnosed in virtually all GBM patients. Treatment of tumor recurrence represents a challenging clinical task. Surgical resection to relief symptoms of mass effect and/or salvage chemotherapy are often considered as last therapeutic option. A new treatment option is urgently needed. Targeted alpha therapy with an intratumoral injection of 213Bi-DOTA-Substance P (SP) or 225Ac-DOTAGA-Substance P has been introduced into the therapeutic armamentarium of recurrent GBM. There are many advantages of using SP such as very high prevalence of increased NK-1 expression in GBM cells, regardless of the degree of malignancy, and expression of the NK-1 receptor system not only on the membrane of cancer cells but also strong expression of NK1 receptors within the tumor neovasculature suggesting concomitant targeting of vascular and neoplastic structures. Radioisotopes with different physical properties, mainly beta-emitting metallic radionuclides, were implemented for brain tumor treatment. Based on their radiophysical properties, however, alpha emitters exhibit more promising properties. In investigator-initiated phase I and II studies, targeted alpha therapy using Bi-213/Ac-225 radiolabeled Substance P for malignant gliomas compare favorably with standard therapy, with the limitation that no large controlled series have so far been generated. Further development should focus on the improvement of the biological and chemical properties of the compound and the application by dedicated catheter systems to improve the intratumoral distribution of the radiopharmaceutical within growth and infiltrative zone of these glial neoplasms. Published by Elsevier Inc.

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Year:  2020        PMID: 32172799     DOI: 10.1053/j.semnuclmed.2019.11.004

Source DB:  PubMed          Journal:  Semin Nucl Med        ISSN: 0001-2998            Impact factor:   4.446


  9 in total

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2.  Novel NK1R-Targeted 68Ga-/177Lu-Radioconjugates with Potential Application against Glioblastoma Multiforme: Preliminary Exploration of Structure-Activity Relationships.

Authors:  Joanna Matalińska; Katarzyna Kosińska; Paweł K Halik; Przemysław Koźmiński; Piotr F J Lipiński; Ewa Gniazdowska; Aleksandra Misicka
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5.  Diffusing alpha-emitters radiation therapy in combination with temozolomide or bevacizumab in human glioblastoma multiforme xenografts.

Authors:  Yossi Nishri; Maayan Vatarescu; Ishai Luz; Lior Epstein; Mirta Dumančić; Sara Del Mare; Amit Shai; Michael Schmidt; Lisa Deutsch; Robert B Den; Itzhak Kelson; Yona Keisari; Lior Arazi; Tomer Cooks; Vered Domankevich
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Review 6.  Novel Receptor Tyrosine Kinase Pathway Inhibitors for Targeted Radionuclide Therapy of Glioblastoma.

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7.  Radiolabeled Gold Nanoseeds Decorated with Substance P Peptides: Synthesis, Characterization and In Vitro Evaluation in Glioblastoma Cellular Models.

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Review 8.  A perspective on the radiopharmaceutical requirements for imaging and therapy of glioblastoma.

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9.  In Vitro Biological Evaluation of Aprepitant Based 177Lu-Radioconjugates.

Authors:  Paweł K Halik; Przemysław Koźmiński; Joanna Matalińska; Piotr F J Lipiński; Aleksandra Misicka; Ewa Gniazdowska
Journal:  Pharmaceutics       Date:  2022-03-10       Impact factor: 6.321

  9 in total

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