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Dive into the research topics where Noeen Malik is active.

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Featured researches published by Noeen Malik.


Applied Radiation and Isotopes | 2011

Radiosynthesis of a new PSMA targeting ligand ([18F]FPy-DUPA-Pep)

Noeen Malik; Hans-Jürgen Machulla; Christoph Solbach; Gordon Winter; Sven N. Reske; Boris D. Zlatopolskiy

Due to the specificity of expression of PSMA (prostate specific membrane antigen) particularly in prostate cancer cells (e.g. LNCaP), numerous PSMA ligands have been synthesized until now. In the current study, we synthesized DUPA-Pep having 2-[3-(1,3-dicarboxypropyl)ureido]pentanedioic acid (DUPA) linked via 8-aminooctanoic acid to two phenylalanine residues and chose 6-[(18)F]fluoronicotinic acid 2,3,5,6-tetrafluorophenyl ester [(18)F]FPy-TFP as a prosthetic group for coupling. [(18)F]FPy-DUPA-Pep was obtained in a radiochemical yield of 48±0.9% (decay uncorrected) within 50 min with a chemical purity of >98%.


The Journal of Nuclear Medicine | 2016

Optimized Peptide Amount and Activity for 90Y-Labeled DOTATATE Therapy

Peter Kletting; Thomas Kull; Christian Maaß; Noeen Malik; Markus Luster; Ambros J. Beer; Gerhard Glatting

In peptide receptor radionuclide therapy with 90Y-labeled DOTATATE, the kidney absorbed dose limits the maximum amount of total activity that can be safely administered in many patients. A higher tumor-to-kidney absorbed dose ratio might be achieved by optimizing the amount of injected peptide and activity, as recent studies have shown different degrees of receptor saturation for normal tissue and tumor. The aim of this work was to develop and implement a modeling method for treatment planning to determine the optimal combination of peptide amount and pertaining therapeutic activity for each patient. Methods: A whole-body physiologically based pharmacokinetic (PBPK) model was developed. General physiologic parameters were taken from the literature. Individual model parameters were fitted to a series (n = 12) of planar γ-camera and serum measurements (111In-DOTATATE) of patients with meningioma or neuroendocrine tumors (NETs). Using the PBPK model and the individually estimated parameters, we determined the tumor, liver, spleen, and red marrow biologically effective doses (BEDs) for a maximal kidney BED (20 Gy2.5) for different peptide amounts and activities. The optimal combination of peptide amount and activity for maximal tumor BED, considering the additional constraint of a red marrow BED less than 1 Gy15, was individually quantified. Results: The PBPK model describes the biokinetic data well considering the criteria of visual inspection, the coefficients of determination, the relative standard errors (<50%), and the correlation of the parameters (<0.8). All fitted parameters were in a physiologically reasonable range but varied considerably between patients, especially tumor perfusion (meningioma, 0.1–1 mL·g−1·min−1, and NETs, 0.02–1 mL·g−1·min−1) and receptor density (meningioma, 5–34 nmol·L−1, and NETs, 7–35 nmol·L−1). Using the proposed method, we identified the optimal amount and pertaining activity to be 76 ± 46 nmol (118 ± 71 μg) and 4.2 ± 1.8 GBq for meningioma and 87 ± 50 nmol (135 ± 78 μg) and 5.1 ± 2.8 GBq for NET patients. Conclusion: The presented work suggests that to achieve higher efficacy and safety for 90Y-DOATATE therapy, both the administered amount of peptide and the activity should be optimized in treatment planning using the proposed method. This approach could also be adapted for therapy with other peptides.


Journal of Controlled Release | 2015

Biodistribution and Delivery Efficiency of Unmodified Tumor-Derived Exosomes

Tyson Smyth; Max Kullberg; Noeen Malik; Peter Smith-Jones; Michael W. Graner; Thomas J. Anchordoquy


Molecular Imaging and Biology | 2015

Radiofluorination of PSMA-HBED via Al 18 F 2+ Chelation and Biological Evaluations In Vitro

Noeen Malik; Benjamin Baur; Gordon Winter; Sven N. Reske; Ambros J. Beer; Christoph Solbach


Journal of Radioanalytical and Nuclear Chemistry | 2010

Nucleophilic aromatic substitution by [18F]fluoride at substituted 2-nitropyridines

Noeen Malik; Christoph Solbach; Wolfgang Voelter; Hans-Jürgen Machulla


Journal of Radioanalytical and Nuclear Chemistry | 2011

Radiofluorination of 2-fluoropyridines by isotopic exchange with [18F]fluoride

Noeen Malik; Wolfgang Voelter; Hans-Jürgen Machulla; Christoph Solbach


Journal of Labelled Compounds and Radiopharmaceuticals | 2012

One pot radiofluorination of a new potential PSMA ligand [Al18F]NOTA‐DUPA‐Pep

Noeen Malik; Boris D. Zlatopolskiy; Hans-Juergen Machulla; Sven N. Reske; Christoph Solbach


Journal of Radioanalytical and Nuclear Chemistry | 2014

Synthesis and labelling of Df-DUPA-Pep with gallium-68 and zirconium-89 as new PSMA ligands

Benjamin Baur; Elena Andreolli; Ehab Al-Momani; Noeen Malik; H.-J. Machulla; Sven N. Reske; Christoph Solbach


Journal of Radioanalytical and Nuclear Chemistry | 2013

Radiosynthesis of ( 18 F)FEt-Tyr-urea-Glu (( 18 F)FEtTUG) as a new PSMA ligand

Ehab Al-Momani; Noeen Malik; H.-J. Machulla; Sven N. Reske; Christoph Solbach


Journal of Radioanalytical and Nuclear Chemistry | 2012

Synthesis of O-[2-[18F]fluoro-3-(2-nitro-1H-imidazole-1-yl)propyl]tyrosine ([18F]FNT]) as a new class of tracer for imaging hypoxia

Noeen Malik; Xian Lin; Dirk Löffler; Bin Shen; Christoph Solbach; Gerald Reischl; Wolfgang Voelter; H.-J. Machulla

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