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Dive into the research topics where Abraham Van Der Spek is active.

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Featured researches published by Abraham Van Der Spek.


Journal of Physical Chemistry B | 2012

Specific and cooperative interactions between oximes and PAMAM dendrimers as demonstrated by 1H NMR study

Seok Ki Choi; Thommey P. Thomas; Pascale R. Leroueil; Alina Kotlyar; Abraham Van Der Spek; James R. Baker

Oximes are important in the treatment of organophosphate (OP) poisoning, but have limited biological half-lives. Complexing these drugs with a macromolecule, such as a dendrimer, could improve their pharmacokinetics. The present study investigates the intermolecular interactions that drive the complexation of oxime-based drug molecules with fifth generation poly(amidoamine) (PAMAM) dendrimers. We performed steady-state binding studies of two molecules, pralidoxime and obidoxime, employing multiple NMR methods, including 1D titration, (1)H-(1)H 2D spectroscopy (COSY, NOESY), and (1)H diffusion-ordered spectroscopy (DOSY). Several important insights were gained in understanding the host-guest interactions occurring between the drug molecules and the polymer. First, the guest molecules bind to the dendrimer macromolecule through a specific interaction rather than through random, hydrophobic encapsulation. Second, this specificity is driven primarily by the electrostatic or H-bond interaction of the oxime at a dendrimer amine site. Also, the average strength for each drug and dendrimer interaction is affected by the surface modification of the polymer. Third, individual binding events between oximes and a dendrimer have a negative cooperative effect on subsequent oxime binding. In summary, this report provides a novel perspective important for designing host systems for drug delivery.


Bioorganic & Medicinal Chemistry Letters | 2009

Human plasma-mediated hypoxic activation of indolequinone-based naloxone pro-drugs.

Baohua Huang; Shengzhuang Tang; Ankur Desai; Xue Min Cheng; Alina Kotlyar; Abraham Van Der Spek; Thommey P. Thomas; James R. Baker

Hypoxia is known to occur in tissues in response to narcotic analgesic therapy using as a result of respiratory depression. The aim of this study was to synthesize a narcotic antagonist pro-drug that can be activated by tissue hypoxia to prevent the damage associated with respiratory depression. We synthesized three different pro-drugs of the narcotic antagonist naloxone utilizing indolequinone as the hypoxia-sensitive moiety. The indolequinone structure in the pro-drugs was designed to have an open reactive point at the N-1 position offering the possibility of further conjugation with macromolecules to modify the bio-availability of these pro-drugs in vivo. A pro-drug (labeled 1) where naloxone and the indolequinone moiety were linked through a carbonate bond was rapidly hydrolyzed in phosphate buffered saline. However, two additional pro-drugs (labeled 2 and 3) having carbamate linkers were stable in phosphate buffered saline for 24h. The reductive release of naloxone from the pro-drugs was achieved in the presence of the bio-reductive enzyme DT-Diaphorase, with about 80% release occurring from the two pro-drugs in 24h. More than 99% of naloxone was released from pro-drug 2 in 30% human plasma, however the release only occurred under hypoxic conditions. This system provides a potential means for feedback control to counter critical respiratory depression induced by narcotic analgesics.


Archive | 1992

Heterogeneity of the Silent Phenotype of Human Butyrylcholinesterase - Identification of Eight New Mutations

Sergio L. Primo-Parmo; Cynthia F. Bartels; Harold Lightstone; Abraham Van Der Spek; Bert N. La Du

The silent phenotype of human butyrylcholinesterase (BChE; E.C. 3.1.1.8) is characterized by the absence or very low levels of enzyme activity. Heterogeneity of this phenotype was recognized soon after the first apparently homozygotes were identified (Goedde and Altland, 1968).


Pediatric Radiology | 2017

Magnetic-resonance-guided biopsy of focal liver lesions

Ethan A. Smith; Jason J. Grove; Abraham Van Der Spek; Marcus D. Jarboe

Image-guided biopsy techniques are widely used in clinical practice. Commonly used methods employ either ultrasound (US) or computed tomography (CT) for image guidance. In certain patients, US or CT guidance may be suboptimal, or even impossible, because of artifacts, suboptimal lesion visualization, or both. We recently began performing magnetic resonance (MR)-guided biopsy of focal liver lesions in select pediatric patients with lesions that are not well visualized by US or CT. This report describes our experience performing MR-guided biopsy of focal liver lesions, with case examples to illustrate innovative techniques and novel aspects of these procedures.


Macromolecules | 2011

Specificity and Negative Cooperativity in Dendrimer–Oxime Drug Complexation

Seok Ki Choi; Pascale R. Leroueil; Ming Hsin Li; Ankur Desai; Hong Zong; Abraham Van Der Spek; James R. Baker


The Lancet | 1985

RESPONSE OF MOYAMOYA DISEASE TO VERAPAMIL

Michael J. McLean; Stephen S. Gebarski; Abraham Van Der Spek; Gary W. Goldstein


Pharmaceutical Research | 2013

Sustained Analgesia Achieved Through Esterase-Activated Morphine Prodrugs Complexed with PAMAM Dendrimer

Brent B. Ward; Baohua Huang; Ankur Desai; Xue Min Cheng; Mark Vartanian; Hong Zong; Xiangyang Shi; Thommey P. Thomas; Alina Kotlyar; Abraham Van Der Spek; Pascale R. Leroueil; James R. Baker


Hastings Center Report | 1989

Mercy, Murder, and Morality

C.J. Berge; Herman H. Meijburg; Abraham Van Der Spek; I. Sluis


Seminars in Anesthesia Perioperative Medicine and Pain | 2004

A perioperative information system: Design and implementation1

Kevin K. Tremper; Michael O’Reilly; Paul E. Kazanjian; Abraham Van Der Spek; Sachin Kheterpal


Bioorganic & Medicinal Chemistry Letters | 2010

Plasma-Mediated Release of Morphine from Synthesized Prodrugs

Thommey P. Thomas; Baohua Huang; Ankur Desai; Hong Zong; Xue Min Cheng; Alina Kotlyar; Pascale R. Leroueil; Thomas Dunham; Abraham Van Der Spek; Brent B. Ward; James R. Baker

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Ankur Desai

University of Michigan

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Hong Zong

University of Michigan

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