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1. Spinal Cord Patterning

Author

Gifford, W.D., primary, Hayashi, M., additional, Sternfeld, M., additional, Tsai, J., additional, Alaynick, W.A., additional, and Pfaff, S.L., additional

Published
2013
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2. Contributors

Author

Akassoglou, K., primary, Alaynick, W.A., additional, Alunni, A., additional, Alvarez-Buylla, A., additional, Ang, S.-L., additional, Appel, B., additional, Arlotta, P., additional, Azim, E., additional, Balice-Gordon, R.J., additional, Bally-Cuif, L., additional, Batista-Brito, R., additional, Baumgardt, M., additional, Begbie, J., additional, Benito-Sipos, J., additional, Bergles, D.E., additional, Brennand, K., additional, Breunig, J.J., additional, Brown, N.L., additional, Buffington, S.A., additional, Campbell, K., additional, Cardona, A.E., additional, Chizhikov, V.V., additional, Coolen, M., additional, Crespo, M., additional, Davies, A.M., additional, De Biase, L.M., additional, Deneen, B., additional, Fahrion, J.K., additional, Fame, R.M., additional, Fishell, G., additional, Foucher, I., additional, Freeman, M.R., additional, Fuentealba, L., additional, Gage, F., additional, Gauthier-Fisher, A., additional, Gifford, W.D., additional, Grande, A., additional, Grove, E.A., additional, Hayashi, M., additional, Hayworth, C.R., additional, Hébert, J., additional, Hemmati-Brivanlou, A., additional, Hobert, O., additional, Hochstim, C., additional, Hufnagel, R.B., additional, Jessen, K.R., additional, Johnson, J.E., additional, Kerschensteiner, M., additional, Kintner, C., additional, Komuro, H., additional, Komuro, Y., additional, Kriegstein, A., additional, Kuert, P.A., additional, Kumada, T., additional, Lai, H.C., additional, Lamb, B., additional, Littner, Y., additional, MacDonald, J.L., additional, Macklis, J.D., additional, Martinez, S., additional, Matise, M., additional, Meijer, D., additional, Meredith, D.M., additional, Merkle, F., additional, Meunier, A., additional, Millen, K.J., additional, Miller, R.H., additional, Miller, F.D., additional, Mirsky, R., additional, Misgeld, T., additional, Molofsky, A.V., additional, Molyneaux, B.J., additional, Monuki, E.S., additional, Nakafuku, M., additional, Nakamura, H., additional, Nave, K.-A., additional, Nelson, B.R., additional, Nelson, C., additional, Nikić, I., additional, Ohno, N., additional, O'Leary, D.D.M., additional, Pfaff, S.L., additional, Pleasure, S.J., additional, Puelles, L., additional, Ransohoff, R.M., additional, Rasband, M.N., additional, Reichert, H., additional, Ross, M.E., additional, Rowitch, D., additional, Rubenstein, J.L.R., additional, Sawamoto, K., additional, Schwab, M.H., additional, Sereda, M.W., additional, Sharma, K., additional, Shen, Q., additional, Shnider, S.J., additional, Siegenthaler, J.A., additional, Sommer, L., additional, Spassky, N., additional, Sternfeld, M., additional, Stocker, A.M., additional, Stork, T., additional, Stott, S.R.W., additional, Svaren, J., additional, Temple, S., additional, Thor, S., additional, Tole, S., additional, Tsai, J., additional, Wegner, M., additional, and Zembrzycki, A., additional

Published
2013
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4. Glycaemic and insulinaemic index of meals in stable obstructive pulmonary disease subjects

Author

Eliraz, A., Sternfeld, M., and Madar, Z.

Subjects
Lung diseases, Obstructive -- Physiological aspects, Adrenocortical hormones -- Physiological aspects, Glucose metabolism -- Analysis
Abstract

Low-glycaemic index (GI) meals control post prandial insulin and glucose levels in stable chronic obstructive pulmonary disease (COPD) patients undergoing glucocorticoid treatment. Low-GI meals administered to diabetic patients regulate plasma glucose concentrations without enhancing insulin demand. High-GI meals decrease the glucose and insulin responses in COPD patients.

Published
1994

7. Promoter elements and alternative splicing in the human ACHE gene

Author

Ben Aziz-Aloya R, Sternfeld M, and Hermona Soreq

Subjects
Genes, RNA Splicing, Molecular Sequence Data, Acetylcholinesterase, Humans, Amino Acid Sequence, Exons, RNA, Messenger, Regulatory Sequences, Nucleic Acid, Promoter Regions, Genetic, Methylation, Protein Processing, Post-Translational, Introns
Published
1993

8. Chapter 16: Promoter elements and alternative splicing in the human ACHE gene

Author

Ben Aziz-Aloya R, Sternfeld M, and Hermona Soreq

Subjects
Genetics, Exon, chemistry.chemical_compound, chemistry, RNA splicing, Alternative splicing, Intron, Cholinergic, Biology, Peptide sequence, Acetylcholinesterase, Gene, Cell biology
Abstract

Publisher Summary A single gene mapped to the 7q22 chromosomal position encodes the ubiquitous acetylcholine hydrolysing enzyme acetylcholinesterase in humans. This unique locus must therefore direct the production of AChE in muscle and nerve, as well as in hemopoietic cells, embryonic tissues, different tumors, and germ cells. Furthermore, the ACHE gene must encode both the major hydrophilic form of AChE expressed in the brain and muscle and the hydrophobic, phosphoinositide (PI)-linked form of the enzyme found in erythrocytes. To reveal the molecular mechanisms underlying this heterogeneous expression, promoter elements and alternative splicing were investigated in the cloned human ACHE gene. The pleiotropic, developmentally-modulated expression and molecular polymorphism of AChE in humans may be attributed to transcriptional, post-transcriptional, and post-translational control mechanisms. These in turn depend on the functioning of multiple nuclear transcriptions and splicing factors and on the association of the different C-terminal peptides in the catalytic subunits with variable structural elements. Understanding of the molecular elements involved in this intricate expression pattern now provides the necessary tools to investigate the roles of AChE in mechanisms of cholinergic function and dysfunction.

Published
1993
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12. Contributors

Author

Akassoglou, K., Alaynick, W.A., Alunni, A., Alvarez-Buylla, A., Ang, S.-L., Appel, B., Arlotta, P., Azim, E., Balice-Gordon, R.J., Bally-Cuif, L., Batista-Brito, R., Baumgardt, M., Begbie, J., Benito-Sipos, J., Bergles, D.E., Brennand, K., Breunig, J.J., Brown, N.L., Buffington, S.A., Campbell, K., Cardona, A.E., Chizhikov, V.V., Coolen, M., Crespo, M., Davies, A.M., De Biase, L.M., Deneen, B., Fahrion, J.K., Fame, R.M., Fishell, G., Foucher, I., Freeman, M.R., Fuentealba, L., Gage, F., Gauthier-Fisher, A., Gifford, W.D., Grande, A., Grove, E.A., Hayashi, M., Hayworth, C.R., Hébert, J., Hemmati-Brivanlou, A., Hobert, O., Hochstim, C., Hufnagel, R.B., Jessen, K.R., Johnson, J.E., Kerschensteiner, M., Kintner, C., Komuro, H., Komuro, Y., Kriegstein, A., Kuert, P.A., Kumada, T., Lai, H.C., Lamb, B., Littner, Y., MacDonald, J.L., Macklis, J.D., Martinez, S., Matise, M., Meijer, D., Meredith, D.M., Merkle, F., Meunier, A., Millen, K.J., Miller, R.H., Miller, F.D., Mirsky, R., Misgeld, T., Molofsky, A.V., Molyneaux, B.J., Monuki, E.S., Nakafuku, M., Nakamura, H., Nave, K.-A., Nelson, B.R., Nelson, C., Nikić, I., Ohno, N., O'Leary, D.D.M., Pfaff, S.L., Pleasure, S.J., Puelles, L., Ransohoff, R.M., Rasband, M.N., Reichert, H., Ross, M.E., Rowitch, D., Rubenstein, J.L.R., Sawamoto, K., Schwab, M.H., Sereda, M.W., Sharma, K., Shen, Q., Shnider, S.J., Siegenthaler, J.A., Sommer, L., Spassky, N., Sternfeld, M., Stocker, A.M., Stork, T., Stott, S.R.W., Svaren, J., Temple, S., Thor, S., Tole, S., Tsai, J., Wegner, M., and Zembrzycki, A.

Published
2013
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20. Overlapping drug interaction sites of human butyrylcholinesterase dissected by site-directed mutagenesis.

Author

Loewenstein-Lichtenstein, Y, Glick, D, Gluzman, N, Sternfeld, M, Zakut, H, and Soreq, H

Abstract

Butyrylcholinesterase [BuChE (acylcholine acyl hydrolase); EC 3.1.1.8] limits the access of drugs, including tacrine, to other proteins. The "atypical" BuChE variant, in which Asp70 at the rim of the active site gorge is substituted by glycine, displayed a more drastically weakened interaction with tacrine than with cocaine, dibucaine, succinylcholine, BW284c51 [1,5-bis(4-allyldimethylammoniumphenyl)pentan-3-one dibromide], or alpha-solanine. To delineate the protein domains that are responsible for this phenomenon, we mutated residues within the rim of the active site gorge, the region parallel to the peripheral site in the homologous enzyme acetylcholinesterase [AChE (acetylcholine acetyl hydrolase); EC 3.1.1.7], the oxyanion hole, and the choline-binding site. When expressed in microinjected Xenopus laevis oocytes, all mutant DNAs yielded comparable amounts of immunoreactive protein products. Most mutants retained catalytic activity close to that of wild-type BuChE and were capable of binding ligands. However, certain modifications in and around the oxyanion hole caused a dramatic loss in activity. The affinities for tacrine were reduced more dramatically than for all other ligands, including cocaine, in both oxyanion hole and choline-binding site mutants. Modified ligand affinities further demonstrated a peripheral site in residues homologous with those of AChE. BuChE mutations that prevented tacrine interactions also hampered its ability to bind other drugs and inhibitors, which suggests a partial overlap of the binding sites. This predicts that in addition to their genetic predisposition to adverse responses to tacrine, homozygous carriers of "atypical" BuChE will be overly sensitive to additional anticholinesterases and especially so when exposed to several anticholinesterases in combination.

Published
1996

21. Transgenic engineering of neuromuscular junctions in Xenopus laevis embryos transiently overexpressing key cholinergic proteins.

Author

Shapira, M, Seidman, S, Sternfeld, M, Timberg, R, Kaufer, D, Patrick, J, and Soreq, H

Abstract

To examine the role of key cholinergic proteins in the formation of neuromuscular junctions (NMJs), we expressed DNAs encoding the mouse muscle nicotinic acetylcholine receptor (nAChR) or human brain and muscle acetylcholinesterase (hAChE) in developing Xenopus laevis embryos. Acetylthiocholine hydrolysis and alpha-bungarotoxin binding in homogenates of transgenic embryos revealed transient overexpression of the respective proteins for at least 4 days postfertilization. Moreover, hAChE injection induced an approximately 2-fold increase in endogenous Xenopus nAChR. Electron microscopy coupled with cytochemical staining for AChE activity revealed that AChE-stained areas, which reached 0.17 microns2 in NMJs of control embryos raised at 21 degrees C, increased up to 0.53 and 0.60 microns2 in nAChR and hAChE transgenics, respectively. These increases coincided with the appearance of a class of large NMJs with average postsynaptic lengths up to 1.8-fold greater than controls. As much as 57% and 34% of the NMJs in animals transgenic for nAChR and hAChE, respectively, displayed AChE activity in nerve terminals in addition to muscle labeling, as compared with 10% nerve-labeled NMJs in control animals. Moreover, area, but not length values, were > 2-fold larger in hAChE-expressing NMJs labeled in their nerve terminals than in those labeled in muscle alone, reflecting a hAChE-induced increase in synaptic cleft width. These findings indicate that modulation of cholinergic neurotransmission in NMJs modifies the features of nerve-muscle connections.

Published
1994
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22. Synaptic and epidermal accumulations of human acetylcholinesterase are encoded by alternative 3'-terminal exons

Author

Seidman, S, Sternfeld, M, Ben Aziz-Aloya, R, Timberg, R, Kaufer-Nachum, D, and Soreq, H

Abstract

Tissue-specific heterogeneity among mammalian acetylcholinesterases (AChE) has been associated with 3' alternative splicing of the primary AChE gene transcript. We have previously demonstrated that human AChE DNA encoding the brain and muscle AChE form and bearing the 3' exon E6 (ACHE-E6) induces accumulation of catalytically active AChE in myotomes and neuromuscular junctions (NMJs) of 2- and 3-day-old Xenopus embryos. Here, we explore the possibility that the 3'-terminal exons of two alternative human AChE cDNA constructs include evolutionarily conserved tissue-recognizable elements. To this end, DNAs encoding alternative human AChE mRNAs were microinjected into cleaving embryos of Xenopus laevis. In contrast to the myotomal expression demonstrated by ACHE-E6, DNA carrying intron 14 and alternative exon E5 (ACHE-I4/E5) promoted punctuated staining of epidermal cells and secretion of AChE into the external medium. Moreover, ACHE-E6-injected embryos displayed enhanced NMJ development, whereas ACHE-I4/E5-derived enzyme was conspicuously absent from muscles and NMJs and its expression in embryos had no apparent effect on NMJ development. In addition, cell-associated AChE from embryos injected with ACHE-I4/E5 DNA was biochemically distinct from that encoded by the muscle-expressible ACHE-E6, displaying higher electrophoretic mobility and greater solubility in low-salt buffer. These findings suggest that alternative 3'-terminal exons dictate tissue-specific accumulation and a particular biological role(s) of AChE, associate the 3' exon E6 with NMJ development, and indicate the existence of a putative secretory AChE form derived from the alternative I4/E5 AChE mRNA.

Published
1995
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23. Gold-induced ileitis.

Author

Geltner, David, Sternfeld, Moshe, Becker, Stuart A., Kori, Moris, Geltner, D, Sternfeld, M, Becker, S A, and Kori, M

Published
1986
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24. Overlapping drug interaction sites of human butyrylcholinesterase dissected by site-directed mutagenesis

Author

Loewenstein-Lichtenstein Y, Glick D, Gluzman N, Sternfeld M, Zakut H, and Hermona Soreq

Subjects
Xenopus laevis, Butyrylcholinesterase, Mutagenesis, Site-Directed, Tacrine, Animals, Humans, Cholinesterase Inhibitors, Benzenaminium, 4,4'-(3-oxo-1,5-pentanediyl)bis(N,N-dimethyl-N-2-propenyl-), Dibromide, Substrate Specificity
Abstract

Butyrylcholinesterase [BuChE (acylcholine acyl hydrolase); EC 3.1.1.8] limits the access of drugs, including tacrine, to other proteins. The "atypical" BuChE variant, in which Asp70 at the rim of the active site gorge is substituted by glycine, displayed a more drastically weakened interaction with tacrine than with cocaine, dibucaine, succinylcholine, BW284c51 [1,5-bis(4-allyldimethylammoniumphenyl)pentan-3-one dibromide], or alpha-solanine. To delineate the protein domains that are responsible for this phenomenon, we mutated residues within the rim of the active site gorge, the region parallel to the peripheral site in the homologous enzyme acetylcholinesterase [AChE (acetylcholine acetyl hydrolase); EC 3.1.1.7], the oxyanion hole, and the choline-binding site. When expressed in microinjected Xenopus laevis oocytes, all mutant DNAs yielded comparable amounts of immunoreactive protein products. Most mutants retained catalytic activity close to that of wild-type BuChE and were capable of binding ligands. However, certain modifications in and around the oxyanion hole caused a dramatic loss in activity. The affinities for tacrine were reduced more dramatically than for all other ligands, including cocaine, in both oxyanion hole and choline-binding site mutants. Modified ligand affinities further demonstrated a peripheral site in residues homologous with those of AChE. BuChE mutations that prevented tacrine interactions also hampered its ability to bind other drugs and inhibitors, which suggests a partial overlap of the binding sites. This predicts that in addition to their genetic predisposition to adverse responses to tacrine, homozygous carriers of "atypical" BuChE will be overly sensitive to additional anticholinesterases and especially so when exposed to several anticholinesterases in combination.

29. Enzyme-Responsive Nanoparticles for Dexamethasone Targeted Delivery to Treat Inflammation in Diabetes.

Author

Schiffmann N, Liang Y, Nemcovsky CE, Almogy M, Halperin-Sternfeld M, Gianneschi NC, Adler-Abramovich L, and Rosen E

Subjects
Rats, Animals, Inflammation drug therapy, Collagen, Dexamethasone pharmacology, Dexamethasone therapeutic use, Diabetes Mellitus, Experimental drug therapy, Diabetes Mellitus, Experimental metabolism, Nanoparticles
Abstract

Diabetes is a global epidemic accompanied by impaired wound healing and increased risk of persistent infections and resistance to standard treatments. Therefore, there is an immense need to develop novel methods to specifically target therapeutics to affected tissues and improve treatment efficacy. This study aims to use enzyme-responsive nanoparticles for the targeted delivery of an anti-inflammatory drug, dexamethasone, to treat inflammation in diabetes. These nanoparticles are assembled from fluorescently-labeled, dexamethasone-loaded peptide-polymer amphiphiles. The nanoparticles are injected in vivo, adjacent to labeled collagen membranes sub-periosteally implanted on the calvaria of diabetic rats. Following their implantation, collagen membrane resorption is linked to inflammation, especially in hyperglycemic individuals. The nanoparticles show strong and prolonged accumulation in inflamed tissue after undergoing a morphological switch into microscale aggregates. Significantly higher remaining collagen membrane area and less inflammatory cell infiltration are observed in responsive nanoparticles-treated rats, compared to control groups injected with free dexamethasone and non-responsive nanoparticles. These factors indicate improved therapeutic efficacy in inflammation reduction. These results demonstrate the potential use of enzyme-responsive nanoparticles as targeted delivery vehicles for the treatment of diabetic and other inflammatory wounds., (© 2023 The Authors. Advanced Healthcare Materials published by Wiley-VCH GmbH.)

Published
2023
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30. Immunomodulatory fibrous hyaluronic acid-Fmoc-diphenylalanine-based hydrogel induces bone regeneration.

Author

Halperin-Sternfeld M, Pokhojaev A, Ghosh M, Rachmiel D, Kannan R, Grinberg I, Asher M, Aviv M, Ma PX, Binderman I, Sarig R, and Adler-Abramovich L

Subjects
Rats, Animals, Cattle, Osteogenesis, X-Ray Microtomography, Calcium pharmacology, Rats, Sprague-Dawley, Bone Regeneration, Periosteum, Tissue Scaffolds chemistry, Hydrogels pharmacology, Hydrogels chemistry, Hyaluronic Acid pharmacology, Hyaluronic Acid therapeutic use
Abstract

Aim: To investigate the potential of an ultrashort aromatic peptide hydrogelator integrated with hyaluronic acid (HA) to serve as a scaffold for bone regeneration., Materials and Methods: Fluorenylmethyloxycarbonyl-diphenylalanine (FmocFF)/HA hydrogel was prepared and characterized using microscopy and rheology. Osteogenic differentiation of MC3T3-E1 preosteoblasts was investigated using Alizarin red, alkaline phosphatase and calcium deposition assays. In vivo, 5-mm-diameter calvarial critical-sized defects were prepared in 20 Sprague-Dawley rats and filled with either FmocFF/HA hydrogel, deproteinized bovine bone mineral, FmocFF/Alginate hydrogel or left unfilled. Eight weeks after implantation, histology and micro-computed tomography analyses were performed. Immunohistochemistry was performed in six rats to assess the hydrogel's immunomodulatory effect., Results: A nanofibrous FmocFF/HA hydrogel with a high storage modulus of 46 KPa was prepared. It supported osteogenic differentiation of MC3T3-E1 preosteoblasts and facilitated calcium deposition. In vivo, the hydrogel implantation resulted in approximately 93% bone restoration. It induced bone deposition not only around the margins, but also generated bony islets along the defect. Elongated M2 macrophages lining at the periosteum-hydrogel interface were observed 1 week after implantation. After 3 weeks, these macrophages were dispersed through the regenerating tissue surrounding the newly formed bone., Conclusions: FmocFF/HA hydrogel can serve as a cell-free, biomimetic, immunomodulatory scaffold for bone regeneration., (© 2022 The Authors. Journal of Clinical Periodontology published by John Wiley & Sons Ltd.)

Published
2023
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31. Stabilizing gelatin-based bioinks under physiological conditions by incorporation of ethylene-glycol-conjugated Fmoc-FF peptides.

Author

Netti F, Aviv M, Dan Y, Rudnick-Glick S, Halperin-Sternfeld M, and Adler-Abramovich L

Subjects
Dipeptides, Ethylenes, Fluorenes, Hydrogels chemistry, Peptides, Phenylalanine, Printing, Three-Dimensional, Tissue Engineering methods, Tissue Scaffolds chemistry, Ethylene Glycol, Gelatin
Abstract

Over the last decade, three-dimensional (3D) printing technologies have attracted the interest of researchers due to the possibility of fabricating tissue- and organ-like structures with similarities to the organ of interest. One of the most widely used materials for the fabrication of bioinks is gelatin (Gel) due to its excellent biocompatibility properties. However, in order to fabricate stable scaffolds under physiological conditions, the most common approach is to use gelatin methacrylate (GelMA) that allows the crosslinking and therefore the stabilization of the hydrogel through UV crosslinking. The crosslinking process can be harmful to cells thus decreasing total cell viability. To overcome the need for post-printing crosslinking, a new approach of bioink formulation was studied, incorporating the Fluorenylmethoxycarbonyl diphenylalanine (Fmoc-FF) peptide into the Gel bioink. However, although Fmoc-FF possesses excellent mechanical properties, the lack of elasticity and viscosity makes it unsuitable for 3D-printing. Here, we demonstrate that covalent conjugation of two different ethylene glycol (EG) motifs to the Fmoc-FF peptide increases the hydrophilicity and elasticity properties, which are essential for 3D-printing. This new approach for bioink formulation avoids the need for any post-printing manufacturing processes, such as chemical or UV crosslinking.

Published
2022
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32. Thixotropic Red Microalgae Sulfated Polysaccharide-Peptide Composite Hydrogels as Scaffolds for Tissue Engineering.

Author

Halperin-Sternfeld M, Netanel Liberman G, Kannan R, Netti F, Ma PX, Arad SM, and Adler-Abramovich L

Abstract

Sulfated polysaccharides of red marine microalgae have recently gained much attention for biomedical applications due to their anti-inflammatory and antioxidant properties. However, their low mechanical properties limit their use in tissue engineering. Herein, to enhance the mechanical properties of the sulfated polysaccharide produced by the red marine microalga, Porphyridium sp. (PS) , it was integrated with the fluorenylmethoxycarbonyl diphenylalanine (FmocFF) peptide hydrogelator. Transparent, stable hydrogels were formed when mixing the two components at a 1:1 ratio in three different concentrations. Electron microscopy showed that all hydrogels exhibited a nanofibrous structure, mimicking the extracellular matrix. Furthermore, the hydrogels were injectable, and tunable mechanical properties were obtained by changing the hydrogel concentration. The composite hydrogels allowed the sustained release of curcumin which was controlled by the change in the hydrogel concentration. Finally, the hydrogels supported MC3T3-E1 preosteoblasts viability and calcium deposition. The synergy between the sulfated polysaccharide, with its unique bioactivities, and FmocFF peptide, with its structural and mechanical properties, bears a promising potential for developing novel tunable scaffolds for tissue engineering that may allow cell differentiation into various lineages.

Published
2022
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33. Mechanical Enhancement and Kinetics Regulation of Fmoc-Diphenylalanine Hydrogels by Thioflavin T.

Author

Tikhonova TN, Rovnyagina NN, Arnon ZA, Yakimov BP, Efremov YM, Cohen-Gerassi D, Halperin-Sternfeld M, Kosheleva NV, Drachev VP, Svistunov AA, Timashev PS, Adler-Abramovich L, and Shirshin EA

Abstract

The self-assembly of peptides is a key direction for fabrication of advanced materials. Novel approaches for fine tuning of macroscopic and microscopic properties of peptide self-assemblies are of a high demand for constructing biomaterials with desired properties. In this work, while studying the kinetics of the Fmoc-Diphenylalanine (Fmoc-FF) dipeptide self-assembly using the Thioflavin T (ThT) dye, we observed that the presence of ThT strongly modifies structural and mechanical properties of the Fmoc-FF hydrogel. Notably, the presence of ThT resulted in a tenfold increase of the gelation time and in the formation of short and dense fibers in the hydrogel. As a result of these morphological alteration higher thermal stability, and most important, tenfold increase of the hydrogel rigidity was achieved. Hence, ThT not only slowed the kinetics of the Fmoc-FF hydrogel formation, but also strongly enhanced its mechanical properties. In this study, we provide a detailed description of the ThT effect on the hydrogel properties and suggest the mechanisms for this phenomenon, paving the way for the novel approach to the control of the peptide hydrogels' micro- and macroscale properties., (© 2021 Wiley-VCH GmbH.)

Published
2021
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34. Dipeptide Nanostructure Assembly and Dynamics via in Situ Liquid-Phase Electron Microscopy.

Author

Gnanasekaran K, Korpanty J, Berger O, Hampu N, Halperin-Sternfeld M, Cohen-Gerassi D, Adler-Abramovich L, and Gianneschi NC

Subjects
Dipeptides, Microscopy, Electron, Transmission, Phenylalanine, Nanostructures, Nanotubes
Abstract

In this paper, we report the in situ growth of FF nanotubes examined via liquid-cell transmission electron microscopy (LCTEM). This direct, high spatial, and temporal resolution imaging approach allowed us to observe the growth of peptide-based nanofibrillar structures through directional elongation. Furthermore, the radial growth profile of FF nanotubes through the addition of monomers perpendicular to the tube axis has been observed in real-time with sufficient resolution to directly observe the increase in diameter. Our study demonstrates that the kinetics, dynamics, structure formation, and assembly mechanism of these supramolecular assemblies can be directly monitored using LCTEM. The performance of the peptides and the assemblies they form can be verified and evaluated using post-mortem techniques including time-of-flight secondary ion mass spectrometry (ToF-SIMS).

Published
2021
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35. Hyaluronic Acid and a Short Peptide Improve the Performance of a PCL Electrospun Fibrous Scaffold Designed for Bone Tissue Engineering Applications.

Author

Rachmiel D, Anconina I, Rudnick-Glick S, Halperin-Sternfeld M, Adler-Abramovich L, and Sitt A

Subjects
Animals, Biocompatible Materials chemistry, Cell Proliferation, Mice, Cell Differentiation, Hyaluronic Acid chemistry, Osteoblasts cytology, Osteogenesis, Peptide Fragments chemistry, Polyesters chemistry, Tissue Scaffolds chemistry
Abstract

Bone tissue engineering is a rapidly developing, minimally invasive technique for regenerating lost bone with the aid of biomaterial scaffolds that mimic the structure and function of the extracellular matrix (ECM). Recently, scaffolds made of electrospun fibers have aroused interest due to their similarity to the ECM, and high porosity. Hyaluronic acid (HA) is an abundant component of the ECM and an attractive material for use in regenerative medicine; however, its processability by electrospinning is poor, and it must be used in combination with another polymer. Here, we used electrospinning to fabricate a composite scaffold with a core/shell morphology composed of polycaprolactone (PCL) polymer and HA and incorporating a short self-assembling peptide. The peptide includes the arginine-glycine-aspartic acid (RGD) motif and supports cellular attachment based on molecular recognition. Electron microscopy imaging demonstrated that the fibrous network of the scaffold resembles the ECM structure. In vitro biocompatibility assays revealed that MC3T3-E1 preosteoblasts adhered well to the scaffold and proliferated, with significant osteogenic differentiation and calcium mineralization. Our work emphasizes the potential of this multi-component approach by which electrospinning, molecular self-assembly, and molecular recognition motifs are combined, to generate a leading candidate to serve as a scaffold for bone tissue engineering.

Published
2021
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36. Surface Modification by Nano-Structures Reduces Viable Bacterial Biofilm in Aerobic and Anaerobic Environments.

Author

Ya'ari S, Halperin-Sternfeld M, Rosin B, and Adler-Abramovich L

Subjects
Aerobiosis, Anaerobiosis, Bacteria metabolism, Coated Materials, Biocompatible chemistry, Enterococcus faecalis drug effects, Enterococcus faecalis metabolism, Enterococcus faecalis physiology, Phenylalanine analogs & derivatives, Phenylalanine chemistry, Streptococcus mutans drug effects, Streptococcus mutans metabolism, Streptococcus mutans physiology, Surface Properties, Anti-Bacterial Agents pharmacology, Bacteria drug effects, Bacterial Adhesion, Bacterial Physiological Phenomena, Biofilms drug effects, Nanostructures chemistry
Abstract

Bacterial biofilm formation on wet surfaces represents a significant problem in medicine and environmental sciences. One of the strategies to prevent or eliminate surface adhesion of organisms is surface modification and coating. However, the current coating technologies possess several drawbacks, including limited durability, low biocompatibility and high cost. Here, we present a simple antibacterial modification of titanium, mica and glass surfaces using self-assembling nano-structures. We have designed two different nano-structure coatings composed of fluorinated phenylalanine via the drop-cast coating technique. We investigated and characterized the modified surfaces by scanning electron microscopy, X-ray diffraction and wettability analyses. Exploiting the antimicrobial property of the nano-structures, we successfully hindered the viability of Streptococcus mutans and Enterococcus faecalis on the coated surfaces in both aerobic and anaerobic conditions. Notably, we found lower bacteria adherence to the coated surfaces and a reduction of 86-99% in the total metabolic activity of the bacteria. Our results emphasize the interplay between self-assembly and antimicrobial activity of small self-assembling molecules, thus highlighting a new approach of biofilm control for implementation in biomedicine and other fields.

Published
2020
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37. Injectable Alginate-Peptide Composite Hydrogel as a Scaffold for Bone Tissue Regeneration.

Author

Ghosh M, Halperin-Sternfeld M, Grinberg I, and Adler-Abramovich L

Abstract

The high demand for tissue engineering scaffolds capable of inducing bone regeneration using minimally invasive techniques prompts the need for the development of new biomaterials. Herein, we investigate the ability of Alginate incorporated with the fluorenylmethoxycarbonyl-diphenylalanine (FmocFF) peptide composite hydrogel to serve as a potential biomaterial for bone regeneration. We demonstrate that the incorporation of the self-assembling peptide, FmocFF, in sodium alginate leads to the production of a rigid, yet injectable, hydrogel without the addition of cross-linking agents. Scanning electron microscopy reveals a nanofibrous structure which mimics the natural bone extracellular matrix. The formed composite hydrogel exhibits thixotropic behavior and a high storage modulus of approximately 10 kPA, as observed in rheological measurements. The in vitro biocompatibility tests carried out with MC3T3-E1 preosteoblast cells demonstrate good cell viability and adhesion to the hydrogel fibers. This composite scaffold can induce osteogenic differentiation and facilitate calcium mineralization, as shown by Alizarin red staining, alkaline phosphatase activity and RT-PCR analysis. The high biocompatibility, excellent mechanical properties and similarity to the native extracellular matrix suggest the utilization of this hydrogel as a temporary three-dimensional cellular microenvironment promoting bone regeneration.

Published
2019
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38. Bio Mimicking of Extracellular Matrix.

Author

Ghosh M, Halperin-Sternfeld M, and Adler-Abramovich L

Subjects
Biocompatible Materials chemistry, Regenerative Medicine, Tissue Scaffolds chemistry, Tissue Scaffolds standards, Biomimetics, Extracellular Matrix chemistry, Tissue Engineering
Abstract

Biomaterials play a critical role in regenerative strategies such as stem cell-based therapies and tissue engineering, aiming to replace, remodel, regenerate, or support damaged tissues and organs. The design of appropriate three-dimensional (3D) scaffolds is crucial for generating bio-inspired replacement tissues. These scaffolds are primarily composed of degradable or non-degradable biomaterials and can be employed as cells, growth factors, or drug carriers. Naturally derived and synthetic biomaterials have been widely used for these purposes, but the ideal biomaterial remains to be found. Researchers from diversified fields have attempted to design and fabricate novel biomaterials, aiming to find novel theranostic approaches for tissue engineering and regenerative medicine. Since no single biomaterial has been found to possess all the necessary characteristics for an ideal performance, over the years scientists have tried to develop composite biomaterials that complement and combine the beneficial properties of multiple materials into a superior matrix. Herein, we highlight the structural features and performance of various biomaterials and their application in regenerative medicine and for enhanced tissue engineering approaches.

Published
2019
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39. Improving the Mechanical Rigidity of Hyaluronic Acid by Integration of a Supramolecular Peptide Matrix.

Author

Aviv M, Halperin-Sternfeld M, Grigoriants I, Buzhansky L, Mironi-Harpaz I, Seliktar D, Einav S, Nevo Z, and Adler-Abramovich L

Subjects
Biocompatible Materials chemical synthesis, Peptides chemical synthesis, Biocompatible Materials chemistry, Extracellular Matrix chemistry, Hyaluronic Acid chemistry, Hydrogels chemistry, Peptides chemistry
Abstract

Hyaluronic acid (HA), a major component of the extracellular matrix, is an attractive material for various medical applications. Yet, its low mechanical rigidity and fast in vivo degradation hinder its utilization. Here, we demonstrate the reinforcement of HA by its integration with a low-molecular-weight peptide hydrogelator to produce a composite hydrogel. The formulation of HA with the fluorenylmethoxycarbonyl diphenylalanine (FmocFF) peptide, one of the most studied self-assembling hydrogel-forming building blocks, showing notable mechanical properties, resulted in the formation of stable, homogeneous hydrogels. Electron microscopy analysis demonstrated a uniform distribution of the two matrices in the composite forms. The composite hydrogels showed improved mechanical properties and stability to enzymatic degradation while maintaining their biocompatibility. Moreover, the storage modulus of the FmocFF/HA composite hydrogels reached up to 25 kPa. The composite hydrogels allowed sustained release of curcumin, a hydrophobic polyphenol showing antioxidant, anti-inflammatory, and antitumor activities. Importantly, the rate of curcumin release was modulated as a function of the concentration of the FmocFF peptide within the hydrogel matrix. This work provides a new approach for conferring mechanical rigidity and stability to HA without the need of cross-linking, thus potentially facilitating its utilization in different clinical applications, such as sustained drug release.

Published
2018
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40. UV Light-Responsive Peptide-Based Supramolecular Hydrogel for Controlled Drug Delivery.

Author

Roth-Konforti ME, Comune M, Halperin-Sternfeld M, Grigoriants I, Shabat D, and Adler-Abramovich L

Subjects
Fluorescein-5-isothiocyanate chemistry, Insulin chemistry, Isothiocyanates chemistry, Drug Delivery Systems methods, Hydrogels chemistry, Peptides chemistry, Ultraviolet Rays
Abstract

Low-molecular-weight self-assembled peptides may serve as promising hydrogelators for drug delivery applications by changing their structural network in response to external stimuli. Herein, inspired by the well-studied low-molecular-weight peptide hydrogelator, fluorenyl-methoxycarbonyl-diphenylalanine (Fmoc-FF), a novel peptide is designed and synthesized to include an ultraviolet (UV)-sensitive phototrigger. Similar to Fmoc-FF, 6-nitroveratryloxycarbonyl-diphenylalanine (Nvoc-FF) self-assembles to form a 3D, self-supporting, nanofibrous hydrogel. The Nvoc-FF hydrogel exhibits good mechanical properties with a storage modulus of 40 kPa. UV irradiation of the Nvoc-FF hydrogel encapsulating insulin-fluorescein isothiocyanate (insulin-FITC) results in the cleavage of Nvoc-FF peptide to produce unmasked FF, thereby facilitating the degradation of the hydrogel and the release of insulin-FITC. This release is in linear correlation to the irradiation time. In the present study, a first insight into this rigid, fibrous, light-responsive hydrogel is provided, allowing the fabrication of a novel drug delivery system for controlled release of large molecules., (© 2018 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published
2018
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41. Arginine-Presenting Peptide Hydrogels Decorated with Hydroxyapatite as Biomimetic Scaffolds for Bone Regeneration.

Author

Ghosh M, Halperin-Sternfeld M, Grigoriants I, Lee J, Nam KT, and Adler-Abramovich L

Subjects
3T3 Cells, Animals, Arginine chemistry, Arginine pharmacology, Biomimetics, Cell Adhesion drug effects, Cell Survival drug effects, Dipeptides chemistry, Dipeptides pharmacology, Durapatite pharmacology, Fluorenes chemistry, Fluorenes pharmacology, Humans, Hydrogels pharmacology, Mice, Peptides pharmacology, Rheology, Tissue Engineering methods, Tissue Scaffolds chemistry, Bone Regeneration, Durapatite chemistry, Hydrogels chemistry, Peptides chemistry
Abstract

Hydrogels are promising candidates for biomimetic scaffolds of the extracellular matrix in tissue engineering applications. However, their use in bone tissue engineering is limited due to their low mechanical properties. In this study, we designed and synthesized multicomponent peptide-based hydrogels composed of fluorenyl-9-methoxycarbonyl diphenylalanine (FmocFF), which contributed to the rigidity and stability of the hydrogel, and Fmoc-arginine (FmocR), which mediated high affinity to hydroxyapatite (HAP) due to the arginine moiety. The new hydrogels composed of nanometric fibril networks were decorated with HAP and demonstrated high mechanical strength with a storage modulus of up to 29 kPa. In addition, the hydrogels supported cell adhesion and in vitro cell viability. These properties suggest using these multicomponent organic-inorganic hydrogels as functional biomaterials for improved bone regeneration.

Published
2017
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42. Dimensional changes of the maxillary sinus following tooth extraction in the posterior maxilla with and without socket preservation.

Author

Levi I, Halperin-Sternfeld M, Horwitz J, Zigdon-Giladi H, and Machtei EE

Subjects
Adult, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Maxillary Sinus anatomy & histology, Tooth Extraction, Tooth Socket surgery
Abstract

Background: Sinus pneumatization is commonly observed following tooth extraction in the posterior maxilla, however, the role of this pneumatization in the overall changes in the vertical bone height is not clear., Purpose: To compare dimensional changes in the alveolar ridge and corresponding maxillary sinus following tooth extraction, with or without socket preservation., Materials and Methods: 42 patients underwent tooth extraction (control group) and 21 patients underwent tooth extraction with socket preservation using DBBM (study group). Panoramic radiographs, prior to and approximately 1 year post extractions were superimposed and matched using a fixed reference unit. The following measurements were performed in the midline of the tooth site: distance of the bone crest to the sinus floor; distance of the sinus floor to the sinus roof and the sagittal circumference of the maxillary., Results: The mean change in the distance from the sinus floor to the sinus roof pre and post operatively was 0.30 mm (±0.10 SE) in the study group and 1.30 mm (±0.27 SE) in the control group (P = .0221). The mean change in the distance from the bone crest to the sinus floor was 0.32 mm (±0.09 SE) in the study group and 1.26 mm (±0.28 SE) in the control group (P = .0019), and the mean change in the sinus sagittal circumference was 37.34 mm (±6.10 SE) and 125.95 mm (±15.60 SE), respectively (P = .0001)., Conclusions: Ridge preservation using bovine derived xenograft might reduce sinus pneumatization along with minimizing crestal bone resorption., (© 2017 Wiley Periodicals, Inc.)

Published
2017
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43. Molecular co-assembly as a strategy for synergistic improvement of the mechanical properties of hydrogels.

Author

Halperin-Sternfeld M, Ghosh M, Sevostianov R, Grigoriants I, and Adler-Abramovich L

Abstract

Molecular self-assembly is a key direction for the fabrication of advanced materials. Yet, the physical properties of the formed assemblies are limited by the inherent characteristics of the specific building blocks. Here, we have applied a co-assembly approach to synergistically modulate the mechanical properties of peptide hydrogels, thereby forming extremely stable and rigid hydrogels.

Published
2017
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44. The Pathogenesis of Implant-Related Reactive Lesions: A Clinical, Histologic and Polarized Light Microscopy Study.

Author

Halperin-Sternfeld M, Sabo E, and Akrish S

Subjects
Dental Implants, Humans, Israel, Retrospective Studies, Gingival Diseases diagnostic imaging, Microscopy, Polarization
Abstract

Background: Peri-implant soft tissue reactive lesions (I-RLs) may jeopardize implant success and survival. To the best of the authors' knowledge, its pathogenesis is unknown. The objective of this study is to conduct a clinicopathologic and polarized light microscopy (PLM) analysis of 14 new I-RLs and compare them with comparable tooth-associated cases (T-RLs) to better understand I-RL pathogenesis., Methods: Fifty-eight new cases of I-RL and T-RL were retrieved from the pathology department archives of Rambam Health Care Campus, Haifa, Israel. Retrospective analysis of histopathologic and clinical features was conducted, documented, and then compared for: 1) I-RL (n = 14), 2) peri-implant pyogenic granuloma (I-PG) (n = 5), 3) peri-implant peripheral giant cell granuloma (I-PGCG) (n = 9), 4) T-RL (n = 44), 5) tooth-associated pyogenic granuloma (T-PG) (n = 21), and 6) tooth-associated peripheral giant cell granuloma (T-PGCG) (n = 23). Presence of foreign bodies was assessed using PLM., Results: Foreign bodies were found more commonly in I-RLs (n = 13/14; 93%) when compared with T-RLs (n = 18/44; 41%), which was a statistically significant difference (P = 0.01) with an odds ratio of 7.9. Microscopically, I-PGCG was associated with: 1) lower multinucleated giant cell count (P = 0.04); 2) lower density of mesenchymal cells (P = 0.05); and 3) more diffuse, non-lobulated stromal morphology (P = 0.001). Clinically, I-RLs were found in patients who were older, and all cases were located in the posterior region: mandible (n = 12/14; 86%) and maxilla (n = 2/14; 14%)., Conclusions: In cases of implant failure, implantation of foreign bodies may play a role with subsequent development of I-PG and I-PGCG-like lesions. Clinicians should be aware of this risk so they can implement measures to minimize adverse implant outcomes.

Published
2016
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45. The association between dental proximal restorations and periodontal disease: A retrospective 10-18 years longitudinal study.

Author

Halperin-Sternfeld M, Saminsky M, Machtei EE, and Horwitz J

Subjects
Dental Marginal Adaptation, Female, Humans, Longitudinal Studies, Male, Middle Aged, Periodontal Index, Retrospective Studies, Dental Restoration, Permanent adverse effects, Periodontal Diseases etiology, Periodontal Diseases therapy
Abstract

Objective: Dental restorations may be plaque retentive. The aim of this study was to evaluate the long-term association between proximal restorations and the incidence and progression of periodontal disease in well-maintained patients., Method and Materials: Probing pocket depths (PPD), bleeding on probing (BOP), and radiographic status of proximal restorations were retrospectively retrieved from files of patients attending a specialist periodontal office. Ill-fitting margins were recorded. The association between these parameters was evaluated at baseline examination (T0), after cause-related therapy (T1) and after ≥ 10 years from T0 (T2), during which supportive periodontal therapy (SPT) was administered, using descriptive statistics, ANOVA-Bonferroni, and chi-square analyses., Results: 1,301 teeth were examined. Mean PPD in unrestored surfaces was 3.7 ± 1.7 mm, 3.1 ± 1.3 mm, and 2.8 ± 1 mm at T0, T1, and T2, respectively. Deeper pockets were found in restored surfaces at those time points with PPD values of 4.4 ± 1.8 mm, 3.6 ± 1.4 mm, and 3.2 ± 1.1 mm, respectively (P < .001). Higher PPD values were found in restored surfaces exhibiting inadequate restorations when compared to restored surfaces with adequate restorations at all time points. These values were 4.9 ± 1.9 mm, 4.1 ± 1.5 mm, and 4 ± 1.7 mm vs 4.3 ± 1.8 mm, 3.6 ± 1.4 mm, and 3.1 ± 1.1 mm, respectively (P < .001)., Conclusion: The present study confirmed that restorations might be detrimental to periodontal health. A significant association between the presence of proximal restorations and the incidence of periodontal disease was observed. This association was more pronounced for inadequate restorations while becoming less significant over time in patients receiving routine SPT.

Published
2016
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46. The association between shallow vestibular depth and peri-implant parameters: a retrospective 6 years longitudinal study.

Author

Halperin-Sternfeld M, Zigdon-Giladi H, and Machtei EE

Subjects
Dental Plaque Index, Female, Humans, Longitudinal Studies, Male, Middle Aged, Periodontal Index, Retrospective Studies, Dental Implants adverse effects
Abstract

Aim: The aim of this study was to retrospectively evaluate the association between shallow vestibular depth (VD) and peri-implant parameters., Material and Methods: Peri-implant parameters were evaluated in 61 periodontal patients under regular supportive periodontal therapy. Clinical parameters included gingival index (GI), plaque index (PI), bleeding on probing (BOP), peri-implant pocket depths (PPD), mucosal recession (MR), relative attachment level (RAL), width and thickness of keratinized mucosa (KMW, KMT) and VD. Radiographic bone level (RBL) was measured on peri-apical radiographs., Results: Sites with shallow VD (≤ 4 mm) were associated with higher MR (0.91 mm versus 0.47 mm, p ≤ 0.009), higher RAL (4.23 mm versus 3.59 mm, p ≤ 0.0001) and higher RBL (2.18 mm versus 1.7 mm, p = 0.05) when compared with adequate vestibular depth sites (VD > 4 mm). Moreover, sites with shallow VD presented lower KMW compared with sites with adequate VD (1.24 mm versus 2.38 mm, respectively, p ≤ 0.0001). Slightly greater BOP, and GI were recorded for the shallow VD compared with adequate sites. According to multivariate analysis, factors that could predict RAL included: VD, GI, age, supporting periodontal therapy, implant type and design., Conclusions: Based on this study, inadequate vestibular depth around dental implants may be associated with increased peri-implant bone loss and mucosal recession. Further prospective and intervention studies will be required to fully understand this phenomenon., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2016
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47. Variables affecting tooth survival and changes in probing depth: a long-term follow-up of periodontitis patients.

Author

Saminsky M, Halperin-Sternfeld M, Machtei EE, and Horwitz J

Subjects
Adult, Age Factors, Aged, Dental Plaque Index, Female, Follow-Up Studies, Health Status, Humans, Longitudinal Studies, Male, Middle Aged, Molar pathology, Periodontal Index, Periodontal Pocket therapy, Prognosis, Proportional Hazards Models, Retrospective Studies, Survival Rate, Tooth Extraction, Treatment Outcome, Periodontal Pocket complications, Tooth Loss etiology
Abstract

Aim: To retrospectively assess tooth-survival rate and its association with patient and oral variables in periodontal office patients, followed up to 18 years., Material and Methods: Patients in a private periodontal office whose files included initial examination (T0 ), reevaluation (TRe ) and ≥ 10 years after T0 (TF ) chartings, and received periodontal therapy and supportive periodontal therapy (SPT) after TRe were included. General health, plaque scores (PI), probing depth (PPD), bleeding on probing (BOP) at six points/tooth, tooth extractions, and SPT visits were extracted from patient files at T0 , TRe , and TF . Descriptive statistics and Cox regression analysis were performed., Results: Fifty patients (mean 26 ± 4 teeth/patient, 1301 teeth) fulfilled inclusion criteria. About 20 and 129 teeth respectively were extracted before/after TRe , 96 of them for periodontal causes. PPD>7 mm at TRe (HR = 17.7, 95%CI 8.6, 36.6), age above 60 years (HR = 3.3, 95%CI 1.5, 7.2), multi-rooted teeth (HR = 1.9, 95%CI 1.2, 3.1) and SPT<3 times/year (HR = 1.8, 95%CI 1.1, 2.9), were the best prognostic factors for tooth loss during follow-up. (p < 0.05, Cox regression analysis). A continuous, statistically significant reduction was observed in mean PPD among teeth that survived follow-up [4.3 ± 1.8 mm, 3.5 ± 1.4 mm, 3.2 ± 1.3 mm, at T0 , TRe , TF , respectively. (p < 0.001, Repeated-measures test)]., Conclusion: Regular SPT was associated with low tooth-loss rates and continuous reductions in probing depth. PPD after initial therapy, age above 60, multi-rooted teeth and infrequent SPT were strong negative prognostic factors for long-term tooth survival among periodontal patients., (© 2015 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2015
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48. Diagnostic accuracy of cone beam computed tomography for dimensional linear measurements in the mandible.

Author

Halperin-Sternfeld M, Machtei EE, and Horwitz J

Subjects
Animals, Confidence Intervals, Female, Gutta-Percha, Mandible anatomy & histology, Sus scrofa, Cone-Beam Computed Tomography, Mandible diagnostic imaging
Abstract

Purpose: To compare linear measurements made on cone beam computed tomography (CBCT) images to direct measurements in ex vivo porcine mandibles., Materials and Methods: Six cross-sectional planes were defined by gutta-percha-filled cavities in seven mandibles. The mandibles were scanned in a CBCT apparatus and later sectioned, using a band saw, through the gutta-percha markers. Next, four direct (DIR) linear measurements were performed for each section with a handheld digital caliper, using the gutta-percha markers as reference points. The corresponding radiographic (RAD) cross sections were then measured using dedicated software. A total of 168 sites were measured. Differences between RAD and DIR measurements [Δ (RAD - DIR)] were calculated for each pair individually., Results: Mean Δ (RAD - DIR) was -0.17 ± 0.53 mm (range, -1.42 to 1.09 mm). CBCT overestimated direct measurements at 36% of the sites; 8% of sites (95% confidence interval, 3.8% to 12.2%) showed errors between +0.5 and +1 mm, and 1.8% (95% confidence interval, -0.2% to 3.9%) showed errors greater than +1 mm., Conclusions: Good correlation was found between CBCT and direct measurements. However, the significant percentage of sites with overestimation of at least 0.5 mm indicates a need for safety margins to be maintained when CBCT is used to plan surgical interventions such as dental implant therapy.

Published
2014
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49. Do we really know how to evaluate tooth prognosis? A systematic review and suggested approach.

Author

Halperin-Sternfeld M and Levin L

Subjects
Decision Making, Disease Progression, Furcation Defects classification, Humans, Logistic Models, Patient Care Planning, Periodontal Index, Predictive Value of Tests, Prognosis, Tooth Mobility classification, Alveolar Bone Loss classification, Periodontitis classification, Tooth Diseases classification, Tooth Extraction statistics & numerical data, Tooth Loss prevention & control
Abstract

Periodontal treatment is based on tooth prognosis evaluation. Different approaches for determining tooth prognosis have been described in the literature. The vast majority are based on clinical and radiographic findings, as well as patient-related factors. The availability of various systems for assigning tooth prognosis complicates both the assignment process and the communication between clinicians regarding patient status and treatment plan. In addition, performance evaluation of several systems reveals that the accuracy of prediction differs between teeth of various conditions in most methods, as well as the factors providing significant predictive power. As a standardized prognostic classification system is still lacking, an overall evaluation based on a uniform dataset could provide an objective comparison of all methods, and help progress towards developing novel approaches. The main features of such approaches should include the selection of predictive factors, their assigned weights in accordance with different tooth conditions, and the estimated period of time applicable for reevaluation of prognosis. In this paper, we propose a different approach for prognosis evaluation, suggesting reevaluating tooth prognosis at several time points during the treatment plan, and taking into consideration some of the most important issues of patient compliance, oral hygiene, and plaque control. The suggested approach attempts to address prognosis from a different perspective, viewing the process as a dynamic and recurring evaluation embedded within each step of the treatment plan. Due to the fact that accurate tooth prognosis evaluation is still (and might forever be) unavailable, a more humble and less aggressive approach should be adopted, trying to preserve more and extract less.

Published
2013
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50. Tooth preservation or implant placement: a systematic review of long-term tooth and implant survival rates.

Author

Levin L and Halperin-Sternfeld M

Subjects
Humans, Tooth Loss therapy, Treatment Outcome, Dental Implants statistics & numerical data
Abstract

Background: For the past few decades, dental implants have served as reliable replacements for missing teeth. However, there is an increasing trend toward replacing diseased teeth with dental implants., Types of Studies Reviewed: The authors conducted a systematic review of long-term survival rates of teeth and implants. They searched the MEDLINE database for relevant publications up to March 2013. They considered studies in which investigators assessed the long-term effectiveness of dental implants or that of tooth preservation. They included only studies that had follow-up periods of 15 years or longer., Results: The authors selected 19 articles for inclusion. Investigators in nine studies assessed the tooth survival rate, whereas investigators in 10 studies assessed the implant survival rate. When comparing the overall long-term (that is, 15 years or more) tooth loss rate with that of implants, the authors observed rates ranging between 3.6 and 13.4 percent and 0 and 33 percent for teeth and implants, respectively. They could not perform a meta-analysis because of the substantial differences between the studies., Practical Implications: The results of this systematic review show that implant survival rates do not exceed those of compromised but adequately treated and maintained teeth, supporting the notion that the decision to extract a tooth and place a dental implant should be made cautiously. Even when a tooth seems to be compromised and requires treatment to be maintained, implant treatment also might require additional surgical procedures that might pose some risks as well. Furthermore, a tooth can be extracted and replaced at any time; however, extraction is a definitive and irreversible treatment.

Published
2013
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