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Dive into the research topics where Tiberiu Mircea Siclovan is active.

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Featured researches published by Tiberiu Mircea Siclovan.


Molecular Imaging | 2011

Nerve-Highlighting Fluorescent Contrast Agents for Image-Guided Surgery

Summer L. Gibbs-Strauss; Khaled Nasr; Kenneth M. Fish; Onkar V. Khullar; Yoshitomo Ashitate; Tiberiu Mircea Siclovan; Bruce Fletcher Johnson; Nicole E. Barnhardt; Cristina Tan Hehir; John V. Frangioni

Nerve damage is the major morbidity of many surgeries, resulting in chronic pain, loss of function, or both. The sparing of nerves during surgical procedures is a vexing problem because surrounding tissue often obscures them. To date, systemically administered nerve-highlighting contrast agents that can be used for nerve-sparing image-guided surgery have not been reported. In the current study, physicochemical and optical properties of 4,4‘-[(2-methoxy-1,4-phenylene)di-(1E)-2,1-ethenediyl]bis-benzenamine (BMB) and a newly synthesized, red-shifted derivative 4-[(1E)-2-[4-[(1E)-2-[4-aminophenyl]ethenyl]-3-methoxyphenyl]ethenyl]-benzonitrile (GE3082) were characterized in vitro and in vivo. Both agents crossed the blood-nerve barrier and blood-brain barrier and rendered myelinated nerves fluorescent after a single systemic injection. Although both BMB and GE3082 also exhibited significant uptake in white adipose tissue, GE3082 underwent a hypsochromic shift in adipose tissue that provided a means to eliminate the unwanted signal using hyperspectral deconvolution. Dose and kinetic studies were performed in mice to determine the optimal dose and drug-imaging interval. The results were confirmed in rat and pig, with the latter used to demonstrate, for the first time, simultaneous fluorescence imaging of blood vessels and nerves during surgery using the FLARE™ (Fluorescence-Assisted Resection and Exploration) imaging system. These results lay the foundation for the development of ideal nerve-highlighting fluorophores for image-guided surgery.


Journal of Histochemistry and Cytochemistry | 2013

Identification of the Protein Target of Myelin-Binding Ligands by Immunohistochemistry and Biochemical Analyses

Anshika Bajaj; Nicole LaPlante; Victoria E. Cotero; Kenneth M. Fish; Roger M. Bjerke; Tiberiu Mircea Siclovan; Cristina Tan Hehir

The ability to visualize myelin is important in the diagnosis of demyelinating disorders and the detection of myelin-containing nerves during surgery. The development of myelin-selective imaging agents requires that a defined target for these agents be identified and that a robust assay against the target be developed to allow for assessment of structure-activity relationships. We describe an immunohistochemical analysis and a fluorescence polarization binding assay using purified myelin basic protein (MBP) that provides quantitative evidence that MBP is the molecular binding partner of previously described myelin-selective fluorescent dyes such as BMB, GE3082, and GE3111.


Molecular Imaging | 2010

Molecular Imaging Agents Specific for the Annulus Fibrosus of the Intervertebral Disk

Summer L. Gibbs-Strauss; Carrie Vooght; Kenneth M. Fish; Khaled Nasr; Tiberiu Mircea Siclovan; Nicole E. Barnhardt; Cristina Tan Hehir; John V. Frangioni

Low back pain is a prevalent medical condition that is difficult to diagnose and treat. Current imaging methods are unable to correlate pain reliably with spinal structures, and surgical removal of painful damaged or degenerating disks is technically challenging. A contrast agent specific for the intervertebral disk could assist in the detection, diagnosis, and surgical treatment of low back pain. The styryl pyridinium (FM) fluorophores were characterized and structure-activity relationships between chemical structure and in vivo uptake were established. Two novel FM fluorophores with improved optical properties for imaging the intervertebral disks were synthesized and evaluated in mice, rats, and pigs. After a single systemic injection, eight of eight FM fluorophores provided high-contrast imaging of the trigeminal ganglia, whereas six of eight provided high-contrast imaging of the dorsal root ganglia. Unexpectedly, three of eight FM fluorophores provided high-contrast imaging of annulus fibrosus tissue of the intervertebral disks, confirmed histologically. We present the first known contrast agent specific for the intervertebral disks and identify the chemical structural motif that mediates uptake. FM fluorophores could be used for image-guided surgery to assist in the removal of intervertebral disk and lay the foundation for derivatives for magnetic resonance imaging and positron emission tomography.


PLOS ONE | 2013

Structure-Activity Relationship of Nerve-Highlighting Fluorophores

Summer L. Gibbs; Yang Xie; Haley L. Goodwill; Khaled Nasr; Yoshitomo Ashitate; Victoria J. Madigan; Tiberiu Mircea Siclovan; Maria I. Zavodszky; Cristina Tan Hehir; John V. Frangioni

Nerve damage is a major morbidity associated with numerous surgical interventions. Yet, nerve visualization continues to challenge even the most experienced surgeons. A nerve-specific fluorescent contrast agent, especially one with near-infrared (NIR) absorption and emission, would be of immediate benefit to patients and surgeons. Currently, there are only three classes of small molecule organic fluorophores that penetrate the blood nerve barrier and bind to nerve tissue when administered systemically. Of these three classes, the distyrylbenzenes (DSBs) are particularly attractive for further study. Although not presently in the NIR range, DSB fluorophores highlight all nerve tissue in mice, rats, and pigs after intravenous administration. The purpose of the current study was to define the pharmacophore responsible for nerve-specific uptake and retention, which would enable future molecules to be optimized for NIR optical properties. Structural analogs of the DSB class of small molecules were synthesized using combinatorial solid phase synthesis and commercially available building blocks, which yielded more than 200 unique DSB fluorophores. The nerve-specific properties of all DSB analogs were quantified using an ex vivo nerve-specific fluorescence assay on pig and human sciatic nerve. Results were used to perform quantitative structure-activity relationship (QSAR) modeling and to define the nerve-specific pharmacophore. All DSB analogs with positive ex vivo fluorescence were tested for in vivo nerve specificity in mice to assess the effect of biodistribution and clearance on nerve fluorescence signal. Two new DSB fluorophores with the highest nerve to muscle ratio were tested in pigs to confirm scalability.


PLOS ONE | 2015

Improved Intraoperative Visualization of Nerves through a Myelin-Binding Fluorophore and Dual-Mode Laparoscopic Imaging

Victoria E. Cotero; Simon Kimm; Tiberiu Mircea Siclovan; Rong Zhang; Evgenia Mikhailovna Kim; Kazuhiro Matsumoto; Tatsuo Gondo; Peter T. Scardino; Siavash Yazdanfar; Vincent P. Laudone; Cristina Tan Hehir

The ability to visualize and spare nerves during surgery is critical for avoiding chronic morbidity, pain, and loss of function. Visualization of such critical anatomic structures is even more challenging during minimal access procedures because the small incisions limit visibility. In this study, we focus on improving imaging of nerves through the use of a new small molecule fluorophore, GE3126, used in conjunction with our dual-mode (color and fluorescence) laparoscopic imaging instrument. GE3126 has higher aqueous solubility, improved pharmacokinetics, and reduced non-specific adipose tissue fluorescence compared to previous myelin-binding fluorophores. Dosing and kinetics were initially optimized in mice. A non-clinical modified Irwin study in rats, performed to assess the potential of GE3126 to induce nervous system injuries, showed the absence of major adverse reactions. Real-time intraoperative imaging was performed in a porcine model. Compared to white light imaging, nerve visibility was enhanced under fluorescence guidance, especially for small diameter nerves obscured by fascia, blood vessels, or adipose tissue. In the porcine model, nerve visualization was observed rapidly, within 5 to 10 minutes post-intravenous injection and the nerve fluorescence signal was maintained for up to 80 minutes. The use of GE3126, coupled with practical implementation of an imaging instrument may be an important step forward in preventing nerve damage in the operating room.


Archive | 2000

Thermally stable polymers, method of preparation, and articles made therefrom

Daniel Joseph Brunelle; Joseph Anthony Suriano; Taeseok Jang; Tiberiu Mircea Siclovan; James Edward Pickett; Gregory Allen O'neil


Archive | 1999

Weatherable block copolyestercarbonates and blends containing them, and method

Tiberiu Mircea Siclovan; Jimmy Lynn Webb; Sterling Bruce Brown; Donald Joseph Buckley; James Edward Pickett; Joseph Anthony Suriano; Paul Dean Sybert; Daniel Joseph Brunelle; Margaret Louise Blohm; Hongyi Zhou; Georgia Dris Fishburn


Archive | 2007

Weatherable, thermostable polymers having improved flow composition

Daniel Joseph Brunelle; Tiberiu Mircea Siclovan; Paul Dean Sybert


Archive | 2003

Compositions and methods for non-invasive imaging of soluble beta-amyloid

Michael Christopher Montalto; Eric Dustin Agdeppa; Tiberiu Mircea Siclovan; Amy Casey Williams


Archive | 2001

METHOD FOR PREPARING COPOLYESTERCARBONATES AND ARTICLES THEREFROM

Joseph Anthony Suriano; Tiberiu Mircea Siclovan; Gregory Allen O'neil; Daniel Joseph Brunelle; Jimmy Lynn Webb

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