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Patel, S. N. D. H., S. S. Ibrahim, and M. A. Yehia, "Flamelet surface density modelling of turbulent deflagrating flames in vented explosions", Journal of Loss Prevention in the Process Industries, vol. 16, no. 6: Elsevier, pp. 451–455, 2003. Abstractfsd_modelling_of_turbulent_deflagrating_flames.pdf

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Patel, D., P. Mohanty, L. Di Biase, J. E. Sanchez, M. H. Shaheen, D. J. Burkhardt, M. Bassouni, J. Cummings, Y. Wang, W. R. Lewis, et al., "Outcomes and complications of catheter ablation for atrial fibrillation in females", Heart Rhythm, vol. 7, no. 2: Elsevier, pp. 167–172, 2010. Abstract
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Patel, M. A., M. H. H. AbouGhaly, and K. Chadwick, "The discovery and investigation of a crystalline solid solution of an active pharmaceutical ingredient", International Journal of Pharmaceutics, vol. 532, no. 1, pp. 166 - 176, 2017. AbstractWebsite

Abstract Understanding the phase behavior of crystal forms is essential in drug formulation development, as physical stability of the active pharmaceutical ingredient (API) is critical to achieving the desired bioavailability. Solvents greatly impact the physical stability of crystalline solids, resulting in a variety of well-known phase transitions, such as hydrate/solvate formation. However, solvent incorporation may also result in the formation of a less-known crystalline solid solutions (CSSs). The identification and characterization of \{CSSs\} and their effect on \{API\} physicochemical properties have not been investigated. This is the first reported instance of a \{CSS\} for an API. An exhaustive study of the phase behavior of the enantiotropically related polymorphs, I and II, of Benzocaine in water and ethanol revealed that Form I formed a \{CSS\} with water below 294.5 K. Construction of the phase diagrams of Forms I and İI\} in water and ethanol revealed that \{CSS\} formation significantly decreased the phase transition temperature between Forms I and İI\} in water. This change resulted from the increased disorder in the lattice of Form I due to the presence of water. This work demonstrates the importance of understanding the formation of \{CSSs\} on the thermodynamic behavior of crystalline pharmaceutical solids.

Patel, M. A., M. H. H. AbouGhaly, J. V. Schryer-Praga, and K. Chadwick, The effect of ionotropic gelation residence time on alginate cross-linking and properties, , vol. 155, pp. 362 - 371, 2017/1/2/. AbstractWebsite

AbstractThe ability to engineer biocompatible polymers with controllable properties is highly desirable. One such approach is to cross-link carbohydrate polymers using ionotropic gelation (IG). Previous studies have investigated the effect of curing time on alginate cross-linking. Herein, we discuss a novel study detailing the effect of IG residence time (IGRT) on the cross-linking of alginate with calcium ions (Ca2+) along with water migration (syneresis) and their subsequent impact on the pharmaceutical properties of alginate particles. IGRT was shown to have a significant effect on particle size, porosity, density, mechanical strength and swelling of calcium alginate particles as well as drug release mechanism. Furthermore, we describe a novel application of electron dispersive spectroscopy (EDS), in conjunction with Fourier Transform- infra red (FT-IR) spectroscopy, to analyze and monitor the changes in Ca2+ concentration during cross-linking. A simple procedure to determine the concentration and distribution of the surface and internal Ca2+ involved in alginate cross-linking was successfully developed.

Patel, C., Z. Xu, E. Shosha, J. Xing, R. Lucas, R. W. Caldwell, R. B. Caldwell, and S. P. Narayanan, "Treatment with polyamine oxidase inhibitor reduces microglial activation and limits vascular injury in ischemic retinopathy.", Biochimica et biophysica acta, vol. 1862, issue 9, pp. 1628-39, 2016 Sep. Abstract

Retinal vascular injury is a major cause of vision impairment in ischemic retinopathies. Insults such as hyperoxia, oxidative stress and inflammation contribute to this pathology. Previously, we showed that hyperoxia-induced retinal neurodegeneration is associated with increased polyamine oxidation. Here, we are studying the involvement of polyamine oxidases in hyperoxia-induced injury and death of retinal vascular endothelial cells. New-born C57BL6/J mice were exposed to hyperoxia (70% O2) from postnatal day (P) 7 to 12 and were treated with the polyamine oxidase inhibitor MDL 72527 or vehicle starting at P6. Mice were sacrificed after different durations of hyperoxia and their retinas were analyzed to determine the effects on vascular injury, microglial cell activation, and inflammatory cytokine profiling. The results of this analysis showed that MDL 72527 treatment significantly reduced hyperoxia-induced retinal vascular injury and enhanced vascular sprouting as compared with the vehicle controls. These protective effects were correlated with significant decreases in microglial activation as well as levels of inflammatory cytokines and chemokines. In order to model the effects of polyamine oxidation in causing microglial activation in vitro, studies were performed using rat brain microvascular endothelial cells treated with conditioned-medium from rat retinal microglia stimulated with hydrogen peroxide. Conditioned-medium from activated microglial cultures induced cell stress signals and cell death in microvascular endothelial cells. These studies demonstrate the involvement of polyamine oxidases in hyperoxia-induced retinal vascular injury and retinal inflammation in ischemic retinopathy, through mechanisms involving cross-talk between endothelial cells and resident retinal microglia.

Patel, A. P., J. L. Fisher, E. Nichols, F. Abd-Allah, J. Abdela, A. Abdelalim, H. N. Abraha, D. Agius, F. Alahdab, and T. Alam, "Global, regional, and national burden of brain and other CNS cancer, 1990–2016: a systematic analysis for the Global Burden of Disease Study 2016", The Lancet Neurology, vol. 18, issue 4: Elsevier, pp. 376-393, 2019. Abstract
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Pasko, D. A., M. D. Churchwell, N. N. Salama, and B. A. Mueller, "Longitudinal Hemodiafilter Performance in Modeled Continuous Renal Replacement Therapy", Blood Purification, vol. 32, issue 2, pp. 82–88, 2011. CU-PDF.pdf
Pasko, D. A., M. D. Churchwell, N. N. Salama, and B. A. Mueller, "Longitudinal Hemodiafilter Performance in Modeled Continuous Renal Replacement Therapy.", Blood Purification, vol. 32, issue 2, pp. 82-88, 2011. pasko.pdf
Pasha, A. M., H. H. Zeineldin, A. S. Al-Sumaiti, M. S. E. Moursi, and E. F. E. Sadaany, "Conservation Voltage Reduction for Autonomous Microgrids Based on V–I Droop Characteristics", IEEE TRANSACTIONS ON SUSTAINABLE ENERGY, vol. 8, issue 3, pp. 1076-1085, 2017.
Pasha, A., H. Zeineldin, E. F. El-Saadany, and S. A. Kaabi, "Optimal allocation of distributed generation for planning master–slave controlled microgrids", IET Generation, Transmission & Distribution, vol. 13, issue 16, pp. 3704-3712, 2019.
Pascalau, E., A. Awad, S. Sakr, and M. Weske, "On Maintaining Consistency of Process Model Variants", Business Process Management Workshops - {BPM} 2010 International Workshops and Education Track, Hoboken, NJ, USA, September 13-15, 2010, Revised Selected Papers, vol. 66: Springer, pp. 289–300, 2010. Abstract
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Parwani, R., and et al, "Odontogenic myxoma in a patient of Turner’s syndrome. ( Prof. Emad Daif was a peer reviewer for this article),", Journal of Cranio-Maxillary Diseases, vol. 3, issue 2, pp. 168, 2014.
Parwani, R., "A case of a rapidly expanding odontogenic myxoma of the mandible. ( Prof. Emad Daif was a peer reviewer for this article),", Journal of Oral Science International, vol. 12, issue 1, pp. 22-26, 2015.
Parwani, A. V., H. A. Hussein, B. I. Rosen, A. Lucchelli, L. Navarro, and L. J. Saif, "Characterization of field strains of group A bovine rotaviruses by using polymerase chain reaction-generated G and P type-specific cDNA probes.", Journal of clinical microbiology, vol. 31, issue 8, pp. 2010-5, 1993 Aug. Abstract

Dot and Northern blot hybridization assays were used to analyze field strains of group A bovine rotaviruses (BRVs) by using nucleic acid probes representing P and G type specificities. The probes were prepared by polymerase chain reaction amplification of hyperdivergent regions of the cloned VP4 (nucleotides 211 to 686) and VP7 (nucleotides 51 to 392) genes from four serotypically distinct (in P or G types) strains of rotaviruses: NCDV (G6, P1), IND (G6, P5), 69M (G8, P10), and Cr (G10, P11). The P and G type cDNA probes were radiolabeled with [32P]dCTP and hybridized with RNA extracted from reference cell culture-passaged rotavirus strains or the field samples. The field samples were obtained from young diarrheic calves from Ohio, Nebraska, Washington State, and Canada. The cDNA probes were specific for their respective G or P types on the basis of analysis of known P and G type reference strains. The G typing analysis of 102 field samples revealed that 36.3% (37 of 102) were G6, 2.9% (3 of 102) were G8, 12.7% (13 of 102) were G10, and 23.5% (24 of 102) were untypeable. The P typing results for 93 samples indicated that 2.2% (2 of 93) were P1 (NCDV-like), 20.4% (19 of 93) were P5 (UK-like), 9.3% (10 of 93) were P11 (B223-like), and 40.8% (38 of 93) were untypeable. This is the first report of the identification among BRV strains in North America of a G type other than G6 or G10. Our report further confirms that G6, P5 rotaviruses are predominant among the BRV field strains that we examined, and the P types of these strains differ from that of the BRV vaccine strain used in the United States (G6, P1). The large number of untypeable G (23.5%) and P (40.8%) types suggests that other or new P and G types exist among BRV field strains.

shawkat parves, M. Attia, and mohamed tawfik, "maxillofacial trauma in Qassim area a five years review", kasr eleini medical jounal, vol. 11, issue 6, pp. 303-311, 2005.
shawkat parves, and M. Attia, "maxillary antrolith on top of traumatic oroantral fistula report of a case", kasr eleini medical jounal, vol. 12, issue 5, pp. 39-42, 2006.
Parthasarathy, S., A. G. Parlos, and A. F. Atiya, "Direct Adaptive Control of Process Systems Using Recurrent Neural Networks", Colloids and Surfaces A-physicochemical and Engineering Aspects, 1992. Abstract
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Parthasarathy, S., A. G. Parlos, and A. F. Atiya, Anticipatory control: A software retrofit for current plant controllers, , 1993. Abstract
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Parthasarathy, S., A. G. Parlos, and A. F. Atiya, Anticipatory control: A software retrofit for current plant controllers, , 1993. Abstract
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Parplys, A. C., J. I. Seelbach, S. Becker, M. Behr, A. Wrona, C. Jend, W. Y. Mansour, S. A. Joosse, H. - W. Stuerzbecher, H. Pospiech, et al., "High levels of RAD51 perturb DNA replication elongation and cause unscheduled origin firing due to impaired CHK1 activation.", Cell cycle (Georgetown, Tex.), vol. 14, issue 19, pp. 3190-202, 2015 Oct 2. Abstractparplys-2015.pdf

In response to replication stress ATR signaling through CHK1 controls the intra-S checkpoint and is required for the maintenance of genomic integrity. Homologous recombination (HR) comprises a series of interrelated pathways that function in the repair of DNA double strand breaks and interstrand crosslinks. In addition, HR, with its key player RAD51, provides critical support for the recovery of stalled forks during replication. High levels of RAD51 are regularly found in various cancers, yet little is known about the effect of the increased RAD51 expression on intra-S checkpoint signaling. Here, we describe a role for RAD51 in driving genomic instability caused by impaired replication and intra-S mediated CHK1 signaling by studying an inducible RAD51 overexpression model as well as 10 breast cancer cell lines. We demonstrate that an excess of RAD51 decreases I-Sce-I mediated HR despite formation of more RAD51 foci. Cells with high RAD51 levels display reduced elongation rates and excessive dormant origin firing during undisturbed growth and after damage, likely caused by impaired CHK1 activation. In consequence, the inability of cells with a surplus of RAD51 to properly repair complex DNA damage and to resolve replication stress leads to higher genomic instability and thus drives tumorigenesis.

Parplys, A. C., J. I. Seelbach, S. Becker, M. Behr, A. Wrona, C. Jend, W. Y. Mansour, S. A. Joosse, H. - W. Stuerzbecher, H. Pospiech, et al., "High levels of RAD51 perturb DNA replication elongation and cause unscheduled origin firing due to impaired CHK1 activation.", Cell cycle (Georgetown, Tex.), vol. 14, issue 19, pp. 3190-202, 2015. Abstract

In response to replication stress ATR signaling through CHK1 controls the intra-S checkpoint and is required for the maintenance of genomic integrity. Homologous recombination (HR) comprises a series of interrelated pathways that function in the repair of DNA double strand breaks and interstrand crosslinks. In addition, HR, with its key player RAD51, provides critical support for the recovery of stalled forks during replication. High levels of RAD51 are regularly found in various cancers, yet little is known about the effect of the increased RAD51 expression on intra-S checkpoint signaling. Here, we describe a role for RAD51 in driving genomic instability caused by impaired replication and intra-S mediated CHK1 signaling by studying an inducible RAD51 overexpression model as well as 10 breast cancer cell lines. We demonstrate that an excess of RAD51 decreases I-Sce-I mediated HR despite formation of more RAD51 foci. Cells with high RAD51 levels display reduced elongation rates and excessive dormant origin firing during undisturbed growth and after damage, likely caused by impaired CHK1 activation. In consequence, the inability of cells with a surplus of RAD51 to properly repair complex DNA damage and to resolve replication stress leads to higher genomic instability and thus drives tumorigenesis.

Parno, D. S., D. Flay, M. Posik, K. Allada, W. Armstrong, T. Averett, F. Benmokhtar, W. Bertozzi, A. Camsonne, M. Canan, et al., Precision measurements of A [n over 1] in the deep inelastic regime, : Elsevier, 2015. Abstract
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Parno, D. S., D. Flay, M. Posik, K. Allada, W. Armstrong, T. Averett, F. Benmokhtar, W. Bertozzi, A. Camsonne, M. Canan, et al., "Precision measurements of A1n in the deep inelastic regime", Physics Letters B, vol. 744: North-Holland, pp. 309–314, 2015. Abstract
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