Your search keyword '"Irina Kerkis"' showing total 134 results

51. Allogeneic Mesenchymal Stem Cell Transplantation in Dogs With Keratoconjunctivitis Sicca

Author

Maura Krähembühl Wanderley Bittencourt, José Paulo Cabral de Vasconcellos, Michele A. Barros, Cristiane Valverde Wenceslau, Bruna P. Morais, Karine Dos Santos Evangelho, Matheus Domingues Bittencourt, Irina Kerkis, João Flávio Panattoni Martins, and Celine Pompeia

Subjects

0301 basic medicine, Single administration, medicine.medical_specialty, business.industry, medicine.medical_treatment, Mesenchymal stem cell, eye diseases, Article, Transplantation, 03 medical and health sciences, 030104 developmental biology, Immunosuppressive drug, medicine.anatomical_structure, Schirmer tear tests, Ophthalmology, medicine, General Earth and Planetary Sciences, KERATOCONJUNCTIVITIS SICCA, Eyelid, sense organs, Adverse effect, business, General Environmental Science

Abstract

Keratoconjunctivitis sicca (KCS) is a dysfunction in tear production associated with clinical signs, which include conjunctival hyperemia, ocular discharge, discomfort, pain, and, eventually, corneal vascularization and pigmentation. Immunosuppressive drugs are routinely administrated for long periods to treat KCS but with side effects and limited results. Evaluation of the clinical benefits of intralacrimal transplantation of allogeneic mesenchymal stem cells (MSCs) in dogs with mild–moderate and severe KCS was done. A total of 24 eyes with KCS from 15 dogs of different breeds were enrolled in the present study. A single transplantation of MSCs (1 × 106) directly into lacrimal glands (dorsal and third eyelid) was performed. The Schirmer tear tests (STTs) and ocular surface improvements were used to assess short- and long-term effects of these cells. The STTs were carried out on day 0 (before MSCs transplantation) and on days 7, 14, 21, and 28, as well as 6 and 12 months after MSC transplantation. Our data demonstrate that allogeneic MSC transplantation in KCS dogs is safe since no adverse effects were observed immediately after transplantation and in short- and long-term follow-ups. A statistically significant increase in the STT and ocular surface improvements was found in all eyes studied. In all the eyes with mild–moderate KCS, STT values reverted to those of healthy eyes, while in eyes with severe KCS, although complete reversion was not found, there was improvement in tear production and in other clinical signs. Our study shows that a single dose of a low number of MSCs can be used to treat KCS in dogs. In contrast to immunosuppressive drug use, MSC transplantation has an effect over a long period (up to 12 months), even after a single administration, and does not require daily drug administration.

Published

2016

52. Induced Pluripotent Stem Cells Derived from Dental Stem Cells: A New Tool for Cellular Therapy

Author

Celine Pompeia, Cristiane Valverde Wenceslau, and Irina Kerkis

Subjects

Endothelial stem cell, Cell therapy, Induced stem cells, Stem cell, Biology, Induced pluripotent stem cell, Regenerative medicine, Embryonic stem cell, Reprogramming, Cell biology

Abstract

Induced pluripotent stem cells (iPSCs) are a type of experimentally produced pluripotent stem cell (PSC), which share similar features with embryonic stem cells (ES) isolated directly from early embryos. Shinya Yamanaka’s lab in Kyoto, Japan was the first to develop iPSCs in 2006 by the introduction of four genes that encode transcription factors of PSC into mouse embryonic fibroblasts—a process known as “reprogramming”. Later on, different animal and human fetal or adult somatic cell types have been converted into iPSCs using this technology, demonstrating similarities and slight differences between iPSCs lines, which are known to depend on the origin of the cells used in reprogramming. The present chapter will provide an overview of iPSCs derived from dental stem cells (DSCs), such as stem cells isolated from apical papilla (SCAPs), stem cells from exfoliated deciduous teeth (SHEDS), from pulp of third molars and adult permanent teeth (DPSCs). We will discuss the origin of the cells used for reprogramming, factors which may favor or hinter the reprogramming process, methods and efficiency of cell reprogramming; the differentiation ability of iPSCs derived from DSCs; their safety, tolerance by the host and regenerative potential in preclinical models, as well as the use of these cells in toxicological studies, disease modeling and drug discovery. The possible use of iPSCs obtained from DSCs as a new tool for regenerative therapy will also be shortly discussed.

Published

2016

53. Derivation and characterization of progenitor stem cells from canine allantois and amniotic fluids at the third trimester of gestation

Author

Cristiane Valverde Wenceslau, Irina Kerkis, M. A. Miglino, R.A. Fernandes, and A.L. Reginato

Subjects

Pathology, medicine.medical_specialty, Amniotic fluid, Progenitor stem cells, Gestational Age, Nerve Tissue Proteins, Amniotic fluids, Biology, Stem cell marker, Immunophenotyping, Canine, Nestin, Andrology, Dogs, Intermediate Filament Proteins, Allantois, Osteogenesis, Pregnancy, Obstetrics and Gynaecology, medicine, Animals, Vimentin, Cells, Cultured, CÉLULAS-TRONCO, Adipogenesis, Keratin-18, medicine.diagnostic_test, Chondrogenic differentiation, Stem Cells, fungi, digestive, oral, and skin physiology, Obstetrics and Gynecology, Cell Differentiation, Amniotic stem cells, Amniotic Fluid, Stem Cell Research, Culture Media, Reproductive Medicine, Cell culture, Amniotic epithelial cells, Allantoic fluids, Amniocentesis, Female, Stem cell, Chondrogenesis, Biomarkers, Developmental Biology, Adult stem cell

Abstract

Fetal tissues are frequently discarded before (amniocentesis) or after birth, which both facilitates stem cell access and helps to overcome ethical concerns. In the present study, we aimed to isolate and characterize stem cells from the allantoic and amniotic fluids (ALF; AMF) of third trimester canine fetuses. This gestation age has not been previously explored for stem cells isolation. The gestational age, cell culture conditions and method of isolation used in this study allowed for the establishment and efficient expansion of ALF and AMF cells. We showed that the majority of ALF and ALF cells express the stem cell markers, such as vimentin, nestin and cytokeratin 18 (CK18). Under appropriate culture conditions AMF derived cells can undergo differentiation into osteogenic, adipogenic, chondrogenic and neuron-like lineages. ALF derived cells showed adipogenic, and chondrogenic potential. Therefore, ALF and AMF cells derived at the third gestation trimester can be qualified as progenitor stem cells, accordingly referred as (alantoic fluid progenitor/stem) ALF PS cells and (amniotic fluid progenitor/stem) AMF PS cells.

Published

2012

54. The Natural Cell-Penetrating Peptide Crotamine Targets Tumor Tissue in Vivo and Triggers a Lethal Calcium-Dependent Pathway in Cultured Cells

Author

Eduardo B. Oliveira, Alexandre Pereira, Helena B. Nader, Jean-Luc Coll, Fabio D. Nascimento, Vitor Oliveira, Irina Kerkis, Mirian A. F. Hayashi, Lucie Sancey, Tetsuo Yamane, Ivarne L.S. Tersariol, and Claire Rome

Subjects

Thapsigargin, Cell Survival, Mice, Nude, Pharmaceutical Science, Antineoplastic Agents, CHO Cells, Cell-Penetrating Peptides, Mitochondrion, Biology, Endoplasmic Reticulum, Calcium in biology, Mice, chemistry.chemical_compound, Cricetulus, Cricetinae, Neoplasms, Crotalid Venoms, Drug Discovery, Tumor Cells, Cultured, Extracellular, Animals, Humans, Calcium Signaling, Membrane Potential, Mitochondrial, Microscopy, Confocal, Cell Death, Endoplasmic reticulum, Crotalus, Microfluorimetry, Flow Cytometry, Xenograft Model Antitumor Assays, Cell biology, Crotamine, HEK293 Cells, chemistry, Molecular Medicine, Calcium, Lysosomes, Injections, Intraperitoneal, Intracellular

Abstract

Our goal was to demonstrate the in vivo tumor specific accumulation of crotamine, a natural peptide from the venom of the South American rattlesnake Crotalus durissus terrificus, which has been characterized by our group as a cell penetrating peptide with a high specificity for actively proliferating cells and with a concentration-dependent cytotoxic effect. Crotamine cytotoxicity has been shown to be dependent on the disruption of lysosomes and subsequent activation of intracellular proteases. In this work, we show that the cytotoxic effect of crotamine also involves rapid intracellular calcium release and loss of mitochondrial membrane potential as observed in real time by confocal microscopy. The intracellular calcium overload induced by crotamine was almost completely blocked by thapsigargin. Microfluorimetry assays confirmed the importance of internal organelles, such as lysosomes and the endoplasmic reticulum, as contributors for the intracellular calcium increase, as well as the extracellular medium. Finally, we demonstrate here that crotamine injected intraperitoneally can efficiently target remote subcutaneous tumors engrafted in nude mice, as demonstrated by a noninvasive optical imaging procedure that permits in vivo real-time monitoring of crotamine uptake into tumor tissue. Taken together, our data indicate that the cytotoxic peptide crotamine can be used potentially for a dual purpose: to target and detect growing tumor tissues and to selectively trigger tumor cell death.

Published

2011

55. Crotamine, a Small Basic Polypeptide Myotoxin from Rattlesnake Venom with Cell-Penetrating Properties

Author

Irina Kerkis and Gandhi Rádis-Baptista

Subjects

Models, Molecular, Myotoxin, Molecular Sequence Data, Antineoplastic Agents, Peptide, Venom, Cell-Penetrating Peptides, Reptilian Proteins, Protein Structure, Secondary, Cell cycle phase, Protein structure, Cell Line, Tumor, Crotalid Venoms, Drug Discovery, Animals, Humans, Amino Acid Sequence, Peptide sequence, Cell Proliferation, Pharmacology, chemistry.chemical_classification, Chemistry, Cell Membrane, Crotamine, Biochemistry, Cell Nucleolus, Nuclear localization sequence, Antimicrobial Cationic Peptides

Abstract

Crotamine, a low molecular weight cationic polypeptide from the venom of the South American rattlesnake Crotalus durissus terrificus is a natural cell-penetrating peptide with functional versatility. The presence of nine lysine residues and three disulfide bonds renders crotamine highly compact, stable and positively charged. Topologically, crotamine adopts an ancient β-defensin fold that is found in diverse families of endogenous and venom polypeptides dedicated to host defense. Crotamine is unique among several classes of bioactive peptides because it possesses both cell penetrating and antimicrobial activities and selective biological action toward some cell types at a given cell cycle phase. Because it can rapidly and efficiently translocate into actively proliferating cells, crotamine is being investigated for labeling highly replicating cells and for use as a chemotherapeutic adjuvant. Peptides derived from crotamine, nucleolar targeting peptides (NrTPs), have been designed and are being studied. NrTPs retain some crotamine properties, such as efficient cellular uptake and preferential nuclear localization whereas they improve upon other properties. For example, NrTPs are smaller than crotamine, show higher preferential nucleolar localization, and better facilitate ZIP-code localization of therapeutic proteins.

Published

2011

56. Early Development and Putative Primordial Germ Cells Characterization in Dogs

Author

Irina Kerkis, Maria Angélica Miglino, Adriana Caroprezo Morini, Cristiane Valverde Wenceslau, Joaquim Mansano Garcia, Daniele dos Santos Martins, Naiara Zoccal Saraiva, and Carlos Eduardo Ambrósio

Subjects

Genetics, Fetus, education.field_of_study, biology, urogenital system, Nucleolus, Embryogenesis, Population, Embryo, Andrology, Endocrinology, medicine.anatomical_structure, Gonocyte, embryonic structures, medicine, biology.protein, Animal Science and Zoology, Antibody, education, Germ cell, Biotechnology

Abstract

Previously, three distinct populations of putative primordial germ cells (PGCs), namely gonocytes, intermediate cells and pre-spermatogonia, have been described in the human foetal testis. According to our knowledge, these PGCs have not been studied in any other species. The aim of our study was to identify similar PGC populations in canine embryos. First, we develop a protocol for canine embryo isolation. Following our protocol, 15 canine embryos at 21-25 days of pregnancy were isolated by ovaryhysterectomy surgery. Our data indicate that dramatic changes occur in canine embryo development and PGCs specification between 21 to 25 days of gestation. At that moment, only two PGC populations with distinct morphology can be identified by histological analyses. Cell population 1 presented round nuclei with prominent nucleolus and a high nuclear to cytoplasm ratio, showing gonocyte morphology. Cell population 2 was often localized at the periphery of the testicular cords and presented typical features of PGC. Both germ cell populations were positively immunostained with anti-human OCT-4 antibody. However, at day 25, all cells of population 1 reacted positively with OCT-4, whereas in population 2, fewer cells were positive for this marker. These two PGCs populations present morphological features similar to gonocytes and intermediate cells from human foetal testis. It is expected that a population of pre-spermatogonia would be observed at later stages of canine foetus development. We also showed that anti-human OCT-4 antibody can be useful to identify canine PGC in vivo.

Published

2011

57. Long-Term Culture of Mouse Embryonic Stem Cell-Derived Adherent Neurospheres and Functional Neurons

Author

Nelson F. Lizier, Irina Kerkis, Alexandre Kerkis, Juliano R. Guerreiro, Antônio Carlos Cassola, Antonio C.M. Camargo, and Mirian A. F. Hayashi

Subjects

Time Factors, Cell Culture Techniques, Biomedical Engineering, Retinoic acid, Medicine (miscellaneous), Bioengineering, Embryoid body, Biology, Models, Biological, Mice, chemistry.chemical_compound, SOX1, Spheroids, Cellular, Neurosphere, Animals, Progenitor cell, Cells, Cultured, Embryoid Bodies, Embryonic Stem Cells, Neurons, Cell Differentiation, Nestin, Embryonic stem cell, In vitro, Cell biology, Gene Expression Regulation, nervous system, chemistry, 1-Alkyl-2-acetylglycerophosphocholine Esterase, Carrier Proteins, Microtubule-Associated Proteins, Biomarkers, Biomedical engineering

Abstract

Innumerous protocols, using the mouse embryonic stem (ES) cells as model for in vitro study of neurons functional properties and features, have been developed. Most of these protocols are short lasting, which, therefore, does not allow a careful analysis of the neurons maturation, aging, and death processes. We describe here a novel and efficient long-lasting protocol for in vitro ES cells differentiation into neuronal cells. It consists of obtaining embryoid bodies, followed by induction of neuronal differentiation with retinoic acid of nonadherent embryoid bodies (three-dimensional model), which further allows their adherence and formation of adherent neurospheres (AN, bi-dimensional model). The AN can be maintained for at least 12 weeks in culture under repetitive mechanical splitting, providing a constant microenvironment (in vitro niche) for the neuronal progenitor cells avoiding mechanical dissociation of AN. The expression of neuron-specific proteins, such as nestin, sox1, beta III-tubulin, microtubule-associated protein 2, neurofilament medium protein, Tau, neuronal nuclei marker, gamma-aminobutyric acid, and 5-hydroxytryptamine, were confirmed in these cells maintained during 3 months under several splitting. Additionally, expression pattern of microtubule-associated proteins, such as lissencephaly (Lis1) and nuclear distribution element-like (Ndel1), which were shown to be essential for differentiation and migration of neurons during embryogenesis, was also studied. As expected, both proteins were expressed in undifferentiated ES cells, AN, and nonrosette neurons, although presenting different spatial distribution in AN. In contrast to previous studies, using cultured neuronal cells derived from embryonic and adult tissues, only Ndel1 expression was observed in the centrosome region of early neuroblasts from AN. Mature neurons, obtained from ES cells in this work, display ionic channels and oscillations of membrane electrical potential typical of electrically excitable cells, which is a characteristic feature of the functional central nervous system (CNS) neurons. Taken together, our study demonstrated that AN are a long-term culture of neuronal cells that can be used to analyze the process of neuronal differentiation dynamics. Thus, the protocol described here provides a new experimental model for studying neurological diseases associated with neuronal differentiation during early development, as well as it represents a novel source of functional cells that can be used as tools for testing the effects of toxins and/or drugs on neuronal cells.

Published

2010

58. Co-Localization of Crotamine with Internal Membranes and Accentuated Accumulation in Tumor Cells

Author

Juliana Mozer Sciani, Nicole Caroline Mambelli-Lisboa, Alvaro R. B. Prieto da Silva, and Irina Kerkis

Subjects

0301 basic medicine, Cell, Pharmaceutical Science, Cell-Penetrating Peptides, Article, Mass Spectrometry, Analytical Chemistry, Mice, 03 medical and health sciences, cell penetrating peptide (CPP), Cell Line, Tumor, Crotalid Venoms, Drug Discovery, medicine, Animals, Physical and Theoretical Chemistry, 030102 biochemistry & molecular biology, Molecular mass, Chemistry, membrane trafficking, Organic Chemistry, co-localization, Intracellular Membranes, molecular imaging, Crotamine, 030104 developmental biology, medicine.anatomical_structure, Membrane, Chemistry (miscellaneous), tumor marker, crotamine, Biophysics, Cell-penetrating peptide, Molecular Medicine, Molecular imaging, Molecular probe, Intracellular

Abstract

Crotamine is a highly cationic; cysteine rich, cross-linked, low molecular mass cell penetrating peptide (CPP) from the venom of the South American rattlesnake. Potential application of crotamine in biomedicine may require its large-scale purification. To overcome difficulties related with the purification of natural crotamine (nCrot) we aimed in the present study to synthesize and characterize a crotamine analog (sCrot) as well investigate its CPP activity. Mass spectrometry analysis demonstrates that sCrot and nCrot have equal molecular mass and biological function—the capacity to induce spastic paralysis in the hind limbs in mice. sCrot CPP activity was evaluated in a wide range of tumor and non-tumor cell tests performed at different time points. We demonstrate that sCrot-Cy3 showed distinct co-localization patterns with intracellular membranes inside the tumor and non-tumor cells. Time-lapse microscopy and quantification of sCrot-Cy3 fluorescence signalss in living tumor versus non-tumor cells revealed a significant statistical difference in the fluorescence intensity observed in tumor cells. These data suggest a possible use of sCrot as a molecular probe for tumor cells, as well as, for the selective delivery of anticancer molecules into these tumors.

Published

2018

59. Quantification of bone mass gain in response to the application of biphasic bioceramics and platelet concentrate in critical-size bone defects

Author

Francisco Henrique Lanna Wykrota, Humberto José Alves, Germán A.B. Mahecha, Ana Carolina Marques Barbosa Oliveira, Irina Kerkis, and Sonja Ellen Lobo

Subjects

Blood Platelets, Male, Ceramics, medicine.medical_specialty, Bone Regeneration, Materials science, Biomedical Engineering, Biophysics, Adipose tissue, Bioengineering, Materials testing, Bone matrix, Osteocytes, Bone and Bones, Biomaterials, Materials Testing, medicine, Animals, Platelet, Platelet concentrate, Bone regeneration, Osteoblasts, Plastic surgery, Adipose Tissue, Bone Substitutes, Rabbits, Biomedical engineering, Bone mass

Abstract

Biphasic bioceramics have been widely indicated for bone reconstruction; however, the real gain in bone mass due to the presence of such biomaterials has not been established yet nor the advantages of its association with platelet concentrate. This study aims at quantifying the volume of bone matrix, osteoblasts, osteocytes, blood vessels and adipose tissue after the application of a biphasic bioceramics composed of 65% hydroxyapatite and 35% beta-tricalcium phosphate. Critical-size bone defects were produced in rabbit femora and reconstructed with bioceramics only, with bioceramics combined with platelet concentrate, with platelet concentrate alone, and with no treatment (blood clot). The quantitative evaluation was performed on histological sections using histomorphometry. Our data provide original evidence that consolidates the indication of bioceramics for clinical bone loss reconstruction. The application of biphasic bioceramics alone led to major bone mass gain and was followed by its association with platelet concentrate. On the other hand, platelet concentrate can contribute to the augmentation and maintenance of the adipose tissue, representing a new field for future applications in plastic surgery.

Published

2008

60. Cytotoxic effects of crotamine are mediated through lysosomal membrane permeabilization

Author

Alexandre Kerkis, Mirian A. F. Hayashi, Ivarne L.S. Tersariol, Eduardo B. Oliveira, Alexandre Pereira, Fabio D. Nascimento, Vitor Oliveira, Irina Kerkis, Helena B. Nader, Tetsuo Yamane, and Gandhi Rádis-Baptista

Subjects

Myotoxin, Antineoplastic Agents, CHO Cells, Biology, Toxicology, Endocytosis, Permeability, Cell membrane, Mice, Cricetulus, Cytosol, Cricetinae, Lysosome, Crotalid Venoms, medicine, Animals, Cytotoxicity, Cell Proliferation, Caspase 3, Cell Membrane, Crotamine, Cysteine Endopeptidases, medicine.anatomical_structure, Biochemistry, Cytoplasm, Lysosomes

Abstract

Crotamine, one of the main toxic components of Crotalus durissus terrificus venom, is a small non-enzymatic basic polypeptide, which causes hind limb paralysis and necrosis of muscle cells. It is well-known that several toxins penetrate into the cytosol through endocytosis, although in many cases the mechanism by which this occurs has not been fully investigated. Recently, using low concentrations of crotamine, we demonstrated the uptake of this toxin into actively proliferative cells via endocytosis, an event that ensues crotamine binding to cell membrane heparan sulfate proteoglycans. Thus, crotamine can be regarded as a cell-penetrating peptide that, additionally, has been shown to be able of delivering some biologically active molecules into various cells. Herein, we investigate one of the mechanisms by which crotamine exerts its cytotoxic effects by following its uptake into highly proliferative cells, as CHO-K1 cells. Crotamine accumulation in the acidic endosomal/lysosomal vesicles was observed within 5 min after treatment of these cells with a cytotoxic concentration of this toxin, a value determined here by classical MTT assay. This accumulation caused disruption of lysosomal vesicles accompanied by the leakage of these vesicles contents into the cytosol. This lysosomal lysis also promoted the release of cysteine cathepsin and an increase of caspase activity in the cytoplasm. This chain of events seems to trigger a cell death process. Overall, our data suggest that lysosomes are the primary targets for crotamine cytotoxicity, a proposal corroborated by the correlation between both the kinetics and concentration-dependence of crotamine accumulation in lysosome compartments and the cytotoxic effects of this protein in CHO-K1 cells. Although crotamine is usually regarded as a myotoxin, we observed that intraperitoneal injection of fluorescently labeled crotamine in living mice led to significant and rapid accumulation of this toxin in the cell cytoplasm of several tissues, suggesting that crotamine cytotoxicity might not be restricted to muscle cells.

Published

2008

61. Reconstruction of Large Cranial Defects in Nonimmunosuppressed Experimental Design With Human Dental Pulp Stem Cells

Author

Roberto D. Fanganiello, Irina Kerkis, Humberto F. Cerruti, Daniela Franco Bueno, André de Mendonça Costa, Nivaldo Alonso, Alexandre Kerkis, Marília Trierveiler Martins, and Maria Rita Passos-Bueno

Subjects

Male, Mature Bone, Cell, Mesenchymal Stem Cell Transplantation, Muscle Development, Parietal Bone, Osteogenesis, Dental pulp stem cells, Deciduous teeth, Animals, Humans, Medicine, Cell Lineage, Rats, Wistar, Tooth, Deciduous, Child, Cells, Cultured, Dental Pulp, Craniofacial surgery, Adipogenesis, business.industry, Mesenchymal stem cell, Cell Differentiation, Membranes, Artificial, Mesenchymal Stem Cells, General Medicine, Anatomy, Fibroblasts, Plastic Surgery Procedures, In vitro, Rats, Disease Models, Animal, medicine.anatomical_structure, Otorhinolaryngology, Surgery, Collagen, Bone Diseases, business, Craniotomy

Abstract

The main aim of this study is to evaluate the capacity of human dental pulp stem cells (hDPSC), isolated from deciduous teeth, to reconstruct large-sized cranial bone defects in nonimmunosuppressed (NIS) rats. To our knowledge, these cells were not used before in similar experiments. We performed two symmetric full-thickness cranial defects (5 x 8 mm) on each parietal region of eight NIS rats. In six of them, the left side was supplied with collagen membrane only and the right side (RS) with collagen membrane and hDPSC. In two rats, the RS had collagen membrane only and nothing was added at the left side (controls). Cells were used after in vitro characterization as mesenchymal cells. Animals were euthanized at 7, 20, 30, 60, and 120 days postoperatively and cranial tissue samples were taken from the defects for histologic analysis. Analysis of the presence of human cells in the new bone was confirmed by molecular analysis. The hDPSC lineage was positive for the four mesenchymal cell markers tested and showed osteogenic, adipogenic, and myogenic in vitro differentiation. We observed bone formation 1 month after surgery in both sides, but a more mature bone was present in the RS. Human DNA was polymerase chain reaction-amplified only at the RS, indicating that this new bone had human cells. The use of hDPSC in NIS rats did not cause any graft rejection. Our findings suggest that hDPSC is an additional cell resource for correcting large cranial defects in rats and constitutes a promising model for reconstruction of human large cranial defects in craniofacial surgery.

Published

2008

62. Membrane-translocating peptides and toxins: from nature to bedside

Author

Mirian A. F. Hayashi, Alexandre Kerkis, Irina Kerkis, Gandhi Rádis Baptista, Yamane Tetsuo, and Alvaro R. B. Prieto da Silva

Subjects

chemistry.chemical_classification, Pore-forming toxin, Chemistry, Antimicrobial peptides, Cell, Peptide, General Chemistry, Transfection, Molecular biology, Crotamine, medicine.anatomical_structure, Biochemistry, medicine, Cell-penetrating peptide, Cytolysin

Abstract

Today, different functional classes of bioactive peptides and toxins isolated from diverse sources of living organisms are known. In medicine, these polypeptides present the potential to be used structurally unmodified or to serve as templates for molecular design of improved derivatives. Here, we refer to members of three classes of remarkable peptides and toxins that act at the cell membranes level and membrane trafficking systems: (i) the binary toxins (ii) the antimicrobial peptides and (iii) the cell penetrating peptides. Binary toxins have been genetically manipulated to generate specific immunotoxins, while antimicrobial peptides are in use as alternative agents against resistant microbes and tumor cells. Cell penetrating peptides have applications as diverse as cell transfection and transport of nanomaterials. Our group is dissecting the capacity of crotamine, a peptide from rattlesnake venom, to translocate cell membranes and use it as a delivery system in the transducing technology and molecular imaging.

Published

2008

63. Chromosome abnormalities in two patients with features of autosomal dominant Robinow syndrome

Author

Rômulo Mombach, Guilherme Colin, Irina Kerkis, Janneke M.M. Weiss, Zan Mustacchi, Ana Cristina Victorino Krepischi-Santos, Carla Rosenberg, Paulo Alberto Otto, Karoly Szuhai, Angela Maria Vianna-Morgante, Rita de Cássia M. Pavanello, Jeroen Knijnenburg, and Juliana F. Mazzeu

Subjects

Chromosome Aberrations, Male, Genetics, Aging, Infant, Dwarfism, medicine.disease, Robinow syndrome, Geography, Spinal Cord, medicine, Humans, Abnormalities, Multiple, Female, Humanities, Genetics (clinical)

Abstract

Juliana F. Mazzeu, Ana Cristina Krepischi-Santos, Carla Rosenberg, Karoly Szuhai, Jeroen Knijnenburg, Janneke M.M. Weiss, Irina Kerkis, Zan Mustacchi, Guilherme Colin, Romulo Mombach, Rita de Cassia M. Pavanello, Paulo A. Otto, and Angela M. Vianna-Morgante* Centro de Estudos do Genoma Humano, Departamento de Genetica e Biologia Evolutiva, Instituto de Biociencias, Universidade de Sao Paulo, Sao Paulo, Brazil Department of Molecular Cell Biology, Leiden University Medical Center, Leiden, The Netherlands Department of Clinical Genetics, Leiden University Medical Center, Leiden, The Netherlands Hospital Infantil Darcy Vargas, Sao Paulo, Brazil Departamento de Genetica Medica, Univille, Joinville, Brazil Centrinho Prefeito Luiz Gomes, Secretaria Municipal de Saude, Joinville, Brazil

Published

2007

64. Neural and mesenchymal stem cells in animal models of Huntington’s disease: past experiences and future challenges

Author

Sabina Glosman, Mônica Santoro Haddad, Cristiane Wenceslau Valverde, and Irina Kerkis

Subjects

Huntingtin, Cell Survival, Medicine (miscellaneous), Clinical uses of mesenchymal stem cells, Review, Biology, Mesenchymal Stem Cell Transplantation, Biochemistry, Genetics and Molecular Biology (miscellaneous), Neural Stem Cells, Huntington's disease, Cancer stem cell, medicine, Animals, Humans, Progenitor cell, Brain, Cell Differentiation, Mesenchymal Stem Cells, Cell Biology, medicine.disease, Neural stem cell, Transplantation, Disease Models, Animal, Huntington Disease, Blood-Brain Barrier, Immunology, Molecular Medicine, Stem cell, Neuroscience

Abstract

Huntington’s disease (HD) is an inherited disease that causes progressive nerve cell degeneration. It is triggered by a mutation in the HTT gene that strongly influences functional abilities and usually results in movement, cognitive and psychiatric disorders. HD is incurable, although treatments are available to help manage symptoms and to delay the physical, mental and behavioral declines associated with the condition. Stem cells are the essential building blocks of life, and play a crucial role in the genesis and development of all higher organisms. Ablative surgical procedures and fetal tissue cell transplantation, which are still experimental, demonstrate low rates of recovery in HD patients. Due to neuronal cell death caused by accumulation of the mutated huntingtin (mHTT) protein, it is unlikely that such brain damage can be treated solely by drug-based therapies. Stem cell-based therapies are important in order to reconstruct damaged brain areas in HD patients. These therapies have a dual role: stem cell paracrine action, stimulating local cell survival, and brain tissue regeneration through the production of new neurons from the intrinsic and likely from donor stem cells. This review summarizes current knowledge on neural stem/progenitor cell and mesenchymal stem cell transplantation, which has been carried out in several animal models of HD, discussing cell distribution, survival and differentiation after transplantation, as well as functional recovery and anatomic improvements associated with these approaches. We also discuss the usefulness of this information for future preclinical and clinical studies in HD.

Published

2015

65. Cell Therapy for Total Limbal Stem Cell Deficiency

Author

Rubens Belfort, Jose Ricardo, Priscila Cristovam, Babyla Monteiro, Irina Kerkis, and Jose Gomes

Subjects

Cell therapy, business.industry, Cancer research, Medicine, business, Limbal stem cell deficiency

Published

2015

66. Differentiation of mouse embryonic stem cells and their hybrids during embryoid body formation

Author

Alexandre Kerkis, Josane Mittmann, Irina Kerkis, Enrico J.C. Santos, Marina Sukoyan, and Cinthia Kawashima

Subjects

Genetics, Tetraploid complementation assay, lcsh:QH426-470, Somatic cell, Karyotype, Embryoid body, differentiation, Biology, pluriopotency, Embryonic stem cell, Cell biology, karyotype, lcsh:Genetics, embryoid bodies, Ploidy, Stem cell, mouse ES-somatic cell hybrids, Molecular Biology, Reprogramming

Abstract

We studied the karyotypes of three hybrid clones of mouse embryonic stem cells and murine splenocytes (two having near diploid and one having near tetraploid chromosome numbers) and the characteristics of their differentiation during the formation of embryoid bodies. The X chromosome originating from embryonic stem cells may be lost in hybrids with a near diploid chromosome number and reprogramming of the "somatic" X may occur. The morphological data we obtained using light and electron microscopy revealed a correlation between the karyotype constitution of hybrid cells and their differentiation during the formation of embryoid bodies. At the beginning of development, the embryoid bodies derived from hybrid cells already showed an advanced degree of differentiation. The production of significant quantities of cartilage was typical for hybrid cells with near tetraploid chromosome numbers. The hybrid cells showed restricted pluripotent capacity and were already committed when they started to differentiate into embryoid bodies.

Published

2002

67. Dental Stem Cells: Risk and Responsibilities

Author

Alexandre Kerkis, Cristiane Valverde Wenceslau, Nelson F. Lizier, and Irina Kerkis

Subjects

Cell type, Dental follicle, animal structures, Mesenchymal stem cell, Embryogenesis, Neural crest, Biology, Cell biology, stomatognathic diseases, Odontoblast, stomatognathic system, embryonic structures, Stem cell, Hox gene

Abstract

In early embryo development, the tooth tissues are originated from the neural crest anatomical site. Neural crest stem cells are considered embryonic-like stem cells, which are maintained under the control of Hox genes. Moreover, they are clonogenic cells and are able to differentiate into various cell types, such as odontoblasts, osteoblasts, chondrocytes, neurons, melanocytes, and the muscles. Following the migration of neural crest stem cells during fetal development, the oral epithelium- and cranial crest-derived mesenchymal cells arise, which next form the dental follicle and dental pulp.

Published

2014

68. Immature Dental Pulp Stem Cells Showed Renotropic and Pericyte-Like Properties in Acute Renal Failure in Rats

Author

Crisitiane Valverde Wenceslau, Dener Madeiro de Souza, Durvanei Augusto Maria, Alexandre Kerkis, Júlio Cesar de Carvalho Balieiro, Irina Kerkis, Niels Olsen Saraiva Câmara, João Flávio Panattoni Martins, and Michele A Barros

Subjects

Pathology, medicine.medical_specialty, Kidney, biology, business.industry, CD44, medicine.disease, Peritubular capillaries, Article, Endothelial stem cell, RATOS, medicine.anatomical_structure, Dental pulp stem cells, biology.protein, medicine, General Earth and Planetary Sciences, Pericyte, Stem cell, business, Acute tubular necrosis, General Environmental Science

Abstract

Acute renal failure (ARF) is a common renal disease that can lead to high mortality. Recovery from ARF occurs with the replacement of necrotic tubular cells by functional tubular epithelial cells and the normalization of microvascular endothelial cell function in the peritubular capillaries. Conventional therapeutic techniques are often ineffective against ARF. Hence, stem cell therapies, which act through multiple trophic and regenerative mechanisms, are encouraging. We investigated the homing of human immature dental pulp stem cells (IDPSCs) after endovenous (EV) or intraperitoneal (IP) injection, in immunocompetent Wistar rats with ARF induced by intramuscular injection of glycerol, without the use of immunosuppression. The cells, which had been cryopreserved for 6 years, were CD105+, CD73+, CD44+, and partly, STRO-1+ and CD146+, and presented unaltered mesoderm differentiation potential. The presence of these cells in the tubular region of the kidney and in the peritubular capillaries was demonstrated. These cells accelerate tubular epithelial cell regeneration through significant increase of Ki-67-immunoreactive cells in damaged kidney. Flow cytometry analysis confirmed that IDPSCs home to the kidneys (EV 34.10% and IP 33.25%); a lower percentage of cells was found in the liver (EV 19.05% and IP 9.10%), in the muscles (EV 6.30% and IP 1.35%), and in the lungs (EV 2.0% and IP 1.85%). After infusion into rat, these cells express pericyte markers, such as CD146+, STRO-1+, and vascular endothelial growth factor (VEGF+). We found that IDPSCs demonstrate renotropic and pericyte-like properties and contributed to restore renal tubule structure in an experimental rat ARF model.

Published

2014

69. State of the Art in the Studies on Crotamine, a Cell Penetrating Peptide from South American Rattlesnake

Author

Alexandre Pereira, Tetsuo Yamane, Paulo Luiz de Sá Júnior, André J. Zaharenko, Mirian A. F. Hayashi, Gandhi Rádis-Baptista, Alvaro R. B. Prieto da Silva, Irina Kerkis, and Alexandre Kerkis

Subjects

Models, Molecular, Cell, Molecular Sequence Data, lcsh:Medicine, Venom, Peptide, Antineoplastic Agents, Review Article, Cell-Penetrating Peptides, Biology, General Biochemistry, Genetics and Molecular Biology, Cell Line, Mice, Anti-Infective Agents, In vivo, Crotalid Venoms, medicine, Animals, Humans, Amino Acid Sequence, Peptide sequence, Melanoma, chemistry.chemical_classification, General Immunology and Microbiology, lcsh:R, Crotalus, General Medicine, South America, In vitro, Crotamine, medicine.anatomical_structure, Biochemistry, chemistry, Immunology, Cell-penetrating peptide

Abstract

Animal venoms comprise a naturally selected cocktail of bioactive peptides/proteins and other molecules, each of which playing a defined role thanks to the highly specific interactions with diverse molecular targets found in the prey. Research focused on isolation, structural, and functional characterizations of novel natural biologics (bioactive peptides/proteins from natural sources) has a long way to go through from the basic science to clinical applications. Herein, we overview the structural and functional characteristics of the myoneurotoxin crotamine, firstly isolated from the South American rattlesnake venom. Crotamine is the first venom peptide classified as a natural cell penetrating and antimicrobial peptide (CPP and AMP) with a more pronounced antifungal activity. In contrast to other known natural CPPs and AMPs, crotamine demonstrates a wide spectrum of biological activities with potential biotechnological and therapeutic values. More recent studies have demonstrated the selectivein vitroanticancer activity of crotamine.In vivo, using a murine melanoma model, it was shown that crotamine delays tumor implantation, inhibits tumor cells proliferation, and also increases the survival of mice engrafted with subcutaneous melanoma. The structural and functional properties and also the possible biotechnological applications of minimized molecules derived from crotamine are also discussed.

Published

2014

70. Generation of Induced Pluripotent Stem Cells from Dental Pulp Somatic Cells

Author

Nelson F. Lizier, Irina Kerkis, and Cristiane Valverde Wenceslau

Subjects

Cell type, medicine.anatomical_structure, Somatic cell, Embryonic Structure, medicine, Neural crest, Connective tissue, Stem cell, Biology, Induced pluripotent stem cell, Embryonic stem cell, Cell biology

Abstract

During early development, human dental pulp is originated from neural crest, which is a transient embryonic structure (Fig. 1). According to current knowledge, neural crest stem cells (NCSCs) have the capacity to self-renewal and display a developmental potential almost the same as embryonic stem (ES) cells (Kerkis and Caplan, 2012). These postmigratory NCSCs generate all craniofacial bones, the majority of the peripheral nervous system cells and tissues, as well as several non-neural cell types, such as smooth muscle cells of the cardiovascular system, pigment cells in the skin, cartilage, connective tissue, corneal epithelium and dental pulp among them. Although postmigratory, postnatal NCSCs are of restricted developmental potential they maintain functional characteristics resembling their embryonic counterparts and an ability to differentiate into a broad spectrum of cell types (Le Douarin et al., 2004, 2007, 2008; Dupin et al., 2007; Le Douarin & Dupin, 2003, 2012).

Published

2013

71. De-Differentiation of Somatic Cells to a Pluripotent State

Author

Cristiane Valverde Wenceslau, Irina Kerkis, Nelson F. Lizier, and AlexandreKerkis

Subjects

Somatic cell, embryonic structures, De differentiation, Biology, Reprogramming, Cell biology

Published

2013

72. Cytotoxic effects of dillapiole on MDA-MB-231 cells involve the induction of apoptosis through the mitochondrial pathway by inducing an oxidative stress while altering the cytoskeleton network

Author

Mariana H. Massaoka, Irina Kerkis, Ivo Lebrun, Kerly Fernanda Mesquita Pasqualoto, Fátima Maria Motter Magri, Aline Vivian Vatti Auada, Alisson L. Matsuo, Diana Aparecida Dias Câmara, Carlos R. Figueiredo, Maurício Temotheo Tavares, Roberto Parise Filho, Paulo Luiz de-Sá-Júnior, Adilson Kleber Ferreira, André Santos Costa, Mariana Celestina Frojuello Costa Bernstorff Damião, and Ricardo A. Azevedo

Subjects

Cell Survival, Apoptosis, Dioxoles, Biology, APOPTOSE, Molecular Dynamics Simulation, medicine.disease_cause, Biochemistry, Gas Chromatography-Mass Spectrometry, Electron Transport Complex IV, chemistry.chemical_compound, Cell Movement, medicine, Cytotoxic T cell, Humans, Calcium Signaling, Cytoskeleton, Actin, Dillapiole, chemistry.chemical_classification, Membrane Potential, Mitochondrial, Reactive oxygen species, Caspase 3, Plant Extracts, General Medicine, Cell cycle, Antineoplastic Agents, Phytogenic, Cell biology, Mitochondria, Allyl Compounds, Oxidative Stress, chemistry, MCF-7 Cells, Drug Screening Assays, Antitumor, Piper, Oxidative stress

Abstract

Breast cancer is the world's leading cause of death among women. This situation imposes an urgent development of more selective and less toxic agents. The use of natural molecular fingerprints as sources for new bioactive chemical entities has proven to be a quite promising and efficient method. Here, we have demonstrated for the first time that dillapiole has broad cytotoxic effects against a variety tumor cells. For instance, we found that it can act as a pro-oxidant compound through the induction of reactive oxygen species (ROS) release in MDA-MB-231 cells. We also demonstrated that dillapiole exhibits anti-proliferative properties, arresting cells at the G0/G1 phase and its antimigration effects can be associated with the disruption of actin filaments, which in turn can prevent tumor cell proliferation. Molecular modeling studies corroborated the biological findings and suggested that dillapiole may present a good pharmacokinetic profile, mainly because its hydrophobic character, which can facilitate its diffusion through tumor cell membranes. All these findings support the fact that dillapiole is a promising anticancer agent.

Published

2013

73. Regeneration of mental nerve of rats with the use of mesenchymal stem cells obtained from dental pulp of human primary teeth

Author

Daniel Martinez Saez, Irina Kerkis, Marcelo Cavenaghi Pereira da Silva, Babyla Geraldes Monteiro, Sonia Regina Yokomizo de Almeida, and Robson Tetsuo Sasaki

Subjects

Pathology, medicine.medical_specialty, business.industry, Regeneration (biology), Mesenchymal stem cell, Genetics, Medicine, business, Molecular Biology, Biochemistry, Mental nerve, Biotechnology

Published

2013

74. A novel strategy of mesenchymal stem cells delivery in the uterus of mares with endometrosis

Author

Alexandre Kerkis, Eduardo Malschitzky, Irina Kerkis, Rodrigo Costa Mattos, Gustavo Henrique Zimmermann Winter, and L. I. Mambelli

Subjects

Pathology, medicine.medical_specialty, Uterus, Endometriosis, Biology, Mesenchymal Stem Cell Transplantation, Food Animals, Cell Movement, Uterus transplantation, medicine, Animals, Horses, Small Animals, Endometrosis, Equine, Mesenchymal stem cell, Uterine horns, Mesenchymal Stem Cells, Transplantation, medicine.anatomical_structure, Animal Science and Zoology, Female, Horse Diseases, Stem cell, Homing (hematopoietic)

Abstract

Mesenchymal stem cells (MSCs), because of their immunomodulation and trophic activities, in addition to their capacity to regenerate damaged tissues, have potential for treatment of many diseases. The success of stem cell therapies depends, in part, on the method of cell delivery, which should provide wide cell distribution and homing in to injured sites. The objective of the present study was to developing a novel strategy for delivery of MSCs into the uterus of mares with endometrosis (degenerative alteration of uterine glands and surrounding stroma). Endometrosis was confirmed in all mares (N = 6) used in this study. To trace multipotent equine adipose tissue-derived MSCs (eAT-MSCs) in endometrial tissue, before transplantation, cells were stained with a fluorescent dye. During a synchronized estrus, the eAT-MSCs (2 × 10(7) diluted in 20 mL of sodium chloride 0.9%) were inoculated into uterus using a simple technique, similar to artificial insemination (AI) in mares. At 7 and 21 days after transplantation, homing of fluorescently labeled eAT-MSCs was observed by confocal microscopy of uterine biopsies collected from the uterine body and in both uterine horns, including glandular and periglandular spaces, in three of four treated mares. Herein, we propose a new method of MSCs delivery in uterus of mares with endometrosis, which was minimally invasive and technically simple.

Published

2012

75. Crotamine: a novel cell-penetrating polypeptide nanocarrier with potential anti-cancer and biotechnological applications

Author

Mirian A F, Hayashi, Eduardo B, Oliveira, Irina, Kerkis, and Richard L, Karpel

Subjects

Base Sequence, Molecular Sequence Data, Gene Transfer Techniques, Cell-Penetrating Peptides, Nanoconjugates, Transfection, Recombinant Proteins, Mice, Inbred C57BL, Mice, Drug Delivery Systems, Cell Line, Tumor, Neoplasms, Nucleic Acids, Crotalid Venoms, Animals, Amino Acid Sequence, Particle Size

Abstract

Crotamine is a basic, 42-residue polypeptide derived from snake venom that has been shown to possess cell-penetrating properties. Crotamine forms nanoparticles with a variety of DNA and RNA molecules, and crotamine-plasmid DNA nanoparticles are selectively delivered into actively proliferating cells in culture or in mice. As such, these nanoparticles could form the basis for a nucleic acid drug-delivery system. Here we describe the preparation, purification, and biochemical and biophysical analysis of venom-derived, recombinant, chemically synthesized, and fluorescent-labeled crotamine; the formation and characterization of crotamine-DNA and -RNA nanoparticles; and the delivery of these nanoparticles into cells and animals.

Published

2012

76. Crotamine: A Novel Cell-Penetrating Polypeptide Nanocarrier with Potential Anti-Cancer and Biotechnological Applications

Author

Eduardo B. Oliveira, Irina Kerkis, Richard L. Karpel, and Mirian A. F. Hayashi

Subjects

business.industry, Cell, RNA, Biotechnology, law.invention, Crotamine, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Biochemistry, Snake venom, law, Nucleic acid, medicine, Recombinant DNA, Nanocarriers, business, DNA

Abstract

Crotamine is a basic, 42-residue polypeptide derived from snake venom that has been shown to possess cell-penetrating properties. Crotamine forms nanoparticles with a variety of DNA and RNA molecules, and crotamine-plasmid DNA nanoparticles are selectively delivered into actively proliferating cells in culture or in mice. As such, these nanoparticles could form the basis for a nucleic acid drug-delivery system. Here we describe the preparation, purification, and biochemical and biophysical analysis of venom-derived, recombinant, chemically synthesized, and fluorescent-labeled crotamine; the formation and characterization of crotamine-DNA and -RNA nanoparticles; and the delivery of these nanoparticles into cells and animals.

Published

2012

77. Stem cells in dental pulp of deciduous teeth

Author

Arnold I. Caplan and Irina Kerkis

Subjects

Pathology, medicine.medical_specialty, Population, Biomedical Engineering, Bioengineering, Biology, Biochemistry, Regenerative medicine, Article, Immunophenotyping, Biomaterials, medicine, Deciduous teeth, Animals, Humans, Stem Cell Niche, Tooth, Deciduous, education, Induced pluripotent stem cell, Dental Pulp, education.field_of_study, Stem Cells, Mesenchymal stem cell, Telomere, Embryonic stem cell, Cell biology, Transplantation, medicine.anatomical_structure, Stem cell

Abstract

Dental pulp from deciduous (baby) teeth, which are discarded after exfoliation, represents an advantageous source of young stem cells. Herein, we discuss the methods of deciduous teeth stem cell (DTSC) isolation and cultivation. We show that based on these methods, at least three different stem cell populations can be identified: a population similar to bone marrow-derived mesenchymal stem cells, an epithelial stem-like cells, and/or a mixed population composed of both cell types. We analyzed the embryonic origin and stem cell niche of DTSCs with respect to the advantages they can provide for their future use in cell therapies and regenerative medicine. In vitro and in vivo differentiation of the DTSC populations, their developmental potential, immunological compatibility, tissue engineering, and transplantation use in studies in animal models are also the focus of the current report. We briefly describe the derivation of induced pluripotent stem (iPS) cells from DTSCs, which can be obtained more easily and efficiently in comparison with human fibroblasts. These iPS cells represent an interesting model for the investigation of pediatric diseases and disorders. The importance of DTSC banking is also discussed.

Published

2011

78. Pluripotent Stem Cells as an In Vitro Model of Neuronal Differentiation

Author

Lygia da Veiga Pereira, Antônio Carlos Cassola, Irina Kerkis, Mirian A. F. Hayashi, Alexandre Kerkis, and Nelson F. Lizier

Subjects

Neuronal differentiation, Library science, Biology, Induced pluripotent stem cell, In vitro model

Abstract

Irina Kerkis1, Mirian A. F. Hayashi2, Nelson F. Lizier1, Antonio C. Cassola3, Lygia V. Pereira4 and Alexandre Kerkis5 1Laboratory of Genetics, Butantan Institute and Department of Morphology and Genetics, Federal University of Sao Paulo, 2Departament of Pharmacology, Federal University of Sao Paulo, 3Department of Physiology and Biophysics, University of Sao Paulo, 4Institute of Biosciences, University of Sao Paulo, 5Celltrovet (Genetica Aplicada), Ltda. Brazil

Published

2011

79. Crotamine toxicity and efficacy in mouse models of melanoma

Author

Aparecida Santo Pietro Pereira, Tetsuo Yamane, Eduardo B. Oliveira, Alexandre Kerkis, Alvaro R. B. Prieto da Silva, Fernando de Sá Silva, Irina Kerkis, Gandhi Rádis-Baptista, A. Pereira, and Mirian A. F. Hayashi

Subjects

Skin Neoplasms, Cell Survival, Antimicrobial peptides, Melanoma, Experimental, Antineoplastic Agents, Pharmacology, Biology, Mice, In vivo, Cell Line, Tumor, Crotalid Venoms, medicine, Cytotoxic T cell, Animals, Humans, Pharmacology (medical), Melanoma, General Medicine, medicine.disease, In vitro, Crotamine, Mice, Inbred C57BL, Disease Models, Animal, Toxicity, Cancer cell, Neoplasm Transplantation

Abstract

Selective anticancer cell activity for both cell-penetrating and cationic antimicrobial peptides has previously been reported. As crotamine possesses activities similar to both of these, this study investigates crotamine's anticancer toxicity in vitro and in vivo.In vitro cancer cell viability was evaluated after treatment with 1 and 5 μg/ml of crotamine. In vivo crotamine cytotoxic effects in C57Bl/6J mice bearing B16-F10 primary cutaneous melanoma were tested, with two groups each containing 35 mice. The crotamine-treated group received 1 μg/day of crotamine per animal, subcutaneously which was well tolerated; the untreated group received a placebo.Crotamine at 5 μg/ml was lethal to B16-F10, Mia PaCa-2 and SK-Mel-28 cells and inoffensive to normal cells. In vivo crotamine treatment over 21 days significantly delayed tumor implantation, inhibited tumor growth and prolonged the lifespan of the mice. Mice in the crotamine-treated group survived at significantly higher rates (n = 30/35) than those in the untreated group (n = 7/35) (significance calculated with the Kaplan-Meier estimator). The average tumor weight in the untreated group was 4.60 g but was only about 0.27 g in the crotamine-treated mice, if detectable.These data warrant further exploration of crotamine as a tumor inhibition compound.

Published

2011

80. Human dental pulp cells: a new source of cell therapy in a mouse model of compressive spinal cord injury

Author

Bruna dos Santos Ramalho, Fernanda Martins de Almeida, Daniel Veloso Cadilhe, Rafaela Fintelman Rodrigues, Suelen Adriani Marques, Daniel Rodrigues Furtado, Ana Maria Blanco Martinez, Irina Kerkis, Lygia da Veiga Pereira, and Stevens K. Rehen

Subjects

medicine.medical_specialty, Pathology, Cell Transplantation, medicine.medical_treatment, Motor Activity, Nerve Fibers, Myelinated, Lesion, Cell therapy, Mice, medicine, Animals, Humans, Spinal cord injury, Spinal Cord Regeneration, Dental Pulp, Neurons, business.industry, Mesenchymal stem cell, Laminectomy, Recovery of Function, medicine.disease, Spinal cord, Embryonic stem cell, Axons, Surgery, medicine.anatomical_structure, Treatment Outcome, Spinal Cord, Models, Animal, Female, Neurology (clinical), CAMUNDONGOS, medicine.symptom, business, Neuroglia, Spinal Cord Compression

Abstract

Strategies aimed at improving spinal cord regeneration after trauma are still challenging neurologists and neuroscientists throughout the world. Many cell-based therapies have been tested, with limited success in terms of functional outcome. In this study, we investigated the effects of human dental pulp cells (HDPCs) in a mouse model of compressive spinal cord injury (SCI). These cells present some advantages, such as the ease of the extraction process, and expression of trophic factors and embryonic markers from both ecto-mesenchymal and mesenchymal components. Young adult female C57/BL6 mice were subjected to laminectomy at T9 and compression of the spinal cord with a vascular clip for 1 min. The cells were transplanted 7 days or 28 days after the lesion, in order to compare the recovery when treatment is applied in a subacute or chronic phase. We performed quantitative analyses of white-matter preservation, trophic-factor expression and quantification, and ultrastructural and functional analysis. Our results for the HDPC-transplanted animals showed better white-matter preservation than the DMEM groups, higher levels of trophic-factor expression in the tissue, better tissue organization, and the presence of many axons being myelinated by either Schwann cells or oligodendrocytes, in addition to the presence of some healthy-appearing intact neurons with synapse contacts on their cell bodies. We also demonstrated that HDPCs were able to express some glial markers such as GFAP and S-100. The functional analysis also showed locomotor improvement in these animals. Based on these findings, we propose that HDPCs may be feasible candidates for therapeutic intervention after SCI and central nervous system disorders in humans.

Published

2011

81. Mesenchymal progenitor cells from canine fetal tissues: yolk sac, liver, and bone marrow

Author

Irina Kerkis, Maria Angélica Miglino, Cristiane Valverde Wenceslau, Nelson F. Lizier, Daniele dos Santos Martins, Graciela Conceição Pignatari, and Carlos Eduardo Ambrósio

Subjects

Pathology, medicine.medical_specialty, Biomedical Engineering, Mice, Nude, Bioengineering, Vimentin, Bone Marrow Cells, Nerve Tissue Proteins, Real-Time Polymerase Chain Reaction, Biochemistry, Biomaterials, Andrology, Nestin, Mice, Dogs, Intermediate Filament Proteins, Microscopy, Electron, Transmission, medicine, Animals, Humans, Yolk sac, Progenitor cell, Cells, Cultured, Yolk Sac, biology, Keratin-18, Mesenchymal stem cell, CD44, Mesenchymal Stem Cells, Haematopoiesis, medicine.anatomical_structure, Hyaluronan Receptors, Liver, EMBRIOLOGIA ANIMAL, Cell culture, embryonic structures, biology.protein, Bone marrow

Abstract

During fetal development, mesenchymal progenitor (MP) cells are co-localized in major hematopoietic territories, such as yolk sac (YS), bone marrow (BM), liver (LV), and others. Studies using mouse and human MP cells isolated from fetus have shown that these cells are very similar but not identical to adult mesenchymal stem cells (MSC). Their differentiation potential is usually restricted to production of highly committed osteogenic and chondrogenic precursors. Such properties of fetal MP cells can be very useful for tissue regeneration, when a great number of committed precursors are required. The objectives of this study were to isolate and characterize MP cells from canine YS, BM, and LV in early and late stages of fetal development. Gestational stage was identified, and cell culture conditions were evaluated for efficient isolation of canine MP cells. All canine fetal MP cells expressed vimentin, nestin, and CD44 proteins. Cytokeratin 18 expression was observed in BM- and LV-MP cells, and vascular endothelial (VE)-cadherin expression was observed only in YS-MP cells. A small number of MP cells (5%) from LV and YS expressed Oct3/4 protein. The differentiation potential of canine fetal MP cells varied significantly: YS- and BM-MP cells differentiated into bone and cartilage, whereas LV-MP cells differentiation was limited to osteogenic fate. None of the canine fetal MP cells were able to differentiate into adipose cells. Our data suggest that canine fetal MP cells are an appropriate in vitro model to study MP biology from hematopoietic territories and they are a source of committed osteogenic and chondrogenic precursors for regenerative medicine.

Published

2011

82. Actual Achievements on Germ Cells and Gametes Derived from Pluripotent Stem Cells

Author

Nelson F. Lizier, Camilla M. Mendes, Irina Kerkis, R. C. Serafim, Alexandre Kerkis, and S. A. S. Fonseca

Subjects

medicine.anatomical_structure, Cell division, Meiosis, Somatic cell, medicine, Gamete, Stem cell, Biology, Induced pluripotent stem cell, Mitosis, Reprogramming, Cell biology

Abstract

In mammals, the specification of GC begins during cleavage; GC first appears near the gut and further migrates to the developing gonads. The lineage of GC is called germ line. They are unique cells, which undergo cell division of two types, mitosis and meiosis, in contrast to somatic cells of mammal’s body, which only divide by mitosis. Accordingly to Fig. 2 following further differentiation GC can be transformed into mature gamete, either eggs or sperm (Adams & McLaren, 2002). There is growing evidence for effects of environmental

Published

2011

83. Feeder-free derivation of induced pluripotent stem cells from human immature dental pulp stem cells

Author

Paulo César Maiorka, Alysson R. Muotri, Nelson F. Lizier, Maria Angélica Miglino, Nélio A. J. Oliveira, Graciela Conceição Pignatari, Patricia Cristina Baleeiro Beltrão-Braga, Cristiane Valverde Wenceslau, and Irina Kerkis

Subjects

Induced Pluripotent Stem Cells, Biomedical Engineering, Cell Culture Techniques, lcsh:Medicine, PEDIATRIA, Mice, Nude, Biology, Mice, Dental pulp stem cells, Animals, Humans, Induced pluripotent stem cell, Child, Cells, Cultured, Dental Pulp, Embryoid Bodies, Stem cell transplantation for articular cartilage repair, Transplantation, lcsh:R, Teratoma, Cell Differentiation, Cell Biology, Cellular Reprogramming, Embryonic stem cell, Cell biology, Multipotent Stem Cell, Karyotyping, Stem cell, Reprogramming, Adult stem cell

Abstract

Induced pluripotent stem cells (iPSCs) can be created by forcing expression of certain genes in fibroblasts or other somatic cell types, reversing them to a pluripotent state similar to that of embryonic stem cells (ESC). Here, we used human immature dental pulp stem cells (hIDPSCs) as an alternative source for creating iPSC. hIDPSCs can be easily isolated from accessible tissue of young and adult patients. hIDPSCs possess a fibroblast-like morphology, retaining characteristics of adult multipotent stem cells. Reprogramming of hIDPSCs was fast, producing primary hIDPSC-iPSC colonies even under feeder-free conditions. hIDPSCs acquired ESC-like morphology, expressed pluripotent markers, possessed stable, normal karyotypes, and demonstrated the ability to differentiated in vitro and in vivo. Our data demonstrate that hIDPSCs-iPSCs offer an advantageous cell system for future cell therapy and basic studies, particularly as a model for pediatric developmental disorders.

Published

2011

84. Biological versatility of crotamine--a cationic peptide from the venom of a South American rattlesnake

Author

Alexandre Kerkis, Irina Kerkis, Gandhi Rádis-Baptista, Fernando de Sá Silva, and Alexandre Pereira

Subjects

Nanotechnology, Venom, Peptide, Antineoplastic Agents, medicine.disease_cause, Crotalid Venoms, medicine, Animals, Humans, Pharmacology (medical), South American rattlesnake, Pharmacology, chemistry.chemical_classification, biology, Toxin, Cell Cycle, Cell Membrane, Crotalus, Intracellular vesicle, General Medicine, South America, biology.organism_classification, Crotamine, Biopharmaceutical, Biochemistry, chemistry, Cell-penetrating peptide, Peptides, Biomarkers

Abstract

Molecules isolated from animals, insects, plants or microorganisms can provide prototypes for design of biopharmaceutical products. Some venom toxins and their derivatives are used in medicine, while others provide templates for development of new drugs.The mild toxin, crotamine, a small basic low-molecular-weight polypeptide purified from the venom of a South American rattlesnake, Crotalus durissus terrificus. Crotamine was discovered more than 50 years ago and only in the past six years has its exceptional biological versatility been demonstrated. Particularly, its cell-penetrating ability, which allows crotamine to cross cell membranes and to accumulate in the nucleus; its use for intracellular vesicle tracking and as a cell cycle marker and its capability for delivering DNA into replicating mammalian cells. Both antimicrobial action and potential selective antitumor activity of crotamine have also been found.Multidisciplinary approaches and pathways of discovery placed crotamine in a rare category of versatile biomolecules, in which concentration, molecular target preference, structural ancestry and specificity toward biological membranes play an integral role.Crotamine is a druggable peptide with high potential for use as an imaging agent for detecting dividing cells, for intracellular delivery of hydrophilic biomolecules, and as an alternative chemotherapeutic compound against aggressive types of cancer.

Published

2010

85. Establishment of a protocol for obtention of neuronal stem cells lineages from the dog olfactory epithelium

Author

Flávio Ribeiro Alves, Irina Kerkis, Maria Angélica Miglino, J. C Delgado, Ricardo Romão Guerra, Carlos Eduardo Ambrósio, Antônio Augusto Nascimento Machado Júnior, and Emerson Ticona Fioretto

Subjects

Pathology, medicine.medical_specialty, education.field_of_study, General Veterinary, Population, Olfactory epithelium, BIOLOGIA CELULAR, Biology, Oligodendrocyte, medicine.anatomical_structure, Cell culture, animal stem cell, medicine, células-tronco animais, cultivo de células caninas, Basal lamina, Progenitor cell, Stem cell, Epitélio olfatório, education, canine cell culture, Immunostaining

Abstract

A morphological and cell culture study from nasal mucosa of dogs was performed in order to establish a protocol to obtain a cell population committed to neuronal lineage, as a proposal for the treatment of traumatic and degenerative lesions in these animals, so that in the future these results could be applied to the human species. Twelve mongrel dogs of 60-day aged pregnancy were collected from urban pound dogs in São Paulo. Tissue from cribriform ethmoidal lamina of the fetuses was collected at necropsy under sterile conditions around 1h to 2h postmortem by uterine sections and sections from the fetal regions described above. Isolated cells of this tissue were added in DMEM/F-12 medium under standard conditions of incubation (5% CO², >37ºC). Cell culture based on isolated cells from biopsies of the olfactory epithelium showed rapid growth when cultured for 24 hours, showing phase-bright sphere cells found floating around the fragments, attached on culture flasks. After 20 days, a specific type of cells, predominantly ellipsoids or fusiform cells was characterized in vitro. The indirect immunofluorescence examination showed cells expressing markers of neuronal precursors (GFAP, neurofilament, oligodendrocyte, and III â-tubulin). The cell proliferation index showed Ki67 immunostaining with a trend to label cell groups throughout the apical region, while PCNA immunostaining label predominantly cell groups lying above the basal lamina. The transmission electron microscopy from the olfactory epithelium of dogs revealed cells with electron-dense cytoplasm and preserving the same distribution as those of positive cell staining for PCNA. Metabolic activity was confirmed by presence of euchromatin in the greatest part of cells. All these aspects give subsidies to support the hypothesis about resident progenitor cells among the basal cells of the olfactory epithelium, committed to renewal of these cell populations, especially neurons. Foi realizado um estudo morfológico e por cultivo celular a partir de células provenientes da mucosa olfatória de cães, como forma de estabelecer um protocolo de cultivo, como uma proposta para o tratamento de lesões traumáticas e nervosas degenerativas nestes animais e futuramente, para que tais resultados possam ser aplicados a espécie humana. Foram utilizados doze cães sem raça definida, a termo, oriundos de castrações do Centro de Controle de Zoonoses de São Paulo. O tecido da lâmina cribiforme do etmóide dos fetos foi coletado sob necropsia, em condições estéreis, 1 a 2 horas post mortem, por meio de incisão uterina e acesso da região fetal supracitada. Depois as células isoladas desse tecido foram adicionadas em médio DMEM/F-12 sob condições padrão (5% CO2, >37ºC). As células obtidas a partir de biópsias do epitélio olfatório de cães apresentaram rápido crescimento após 24 horas de cultivo, demonstrando morfologia esférica, sendo encontradas flutuando ao redor do fragmento aderido à garrafa de cultura. Após 20 dias, foram verificados tipos celulares específicos, predominantemente elipsóides ou fusiformes, foram observadas in vitro. Sob avaliação por imunofluorescência indireta observaram-se células com expressão positiva para marcadores de precursores neuronais (GFAP, Neurofilamentos, oligodendrócitos e â-tubulina III). O índice de proliferação celular mostrou-se positivo para Ki67 com uma tendência de marcação de grupos celulares ao longo da região apical, enquanto a imunomarcação para PCNA mostrou-se predominantemente em grupos celulares residentes sobre a lâmina basal. A microscopia eletrônica de transmissão do epitélio olfatório de cães revelou células com citoplasma eletrodenso e mesma distribuição das células marcadas positivamente para PCNA. A atividade metabólica foi confirmada pela presença de eucromatina em muitas regiões celulares. Todos estes aspectos sustentam a hipotese sobre a presença de células progenitoras residentes entre as células basais do epitélio olfatório comprometidas com a renovação desse epitélio, particularmente a população de neurônios.

Published

2010

86. Successful transplant of mesenchymal stem cells in induced osteonecrosis of the ovine femoral head: preliminary results

Author

Eduardo Harry Birgel Júnior, Maria Angélica Miglino, Matheus Levi Tajra Feitosa, Irina Kerkis, Patricia Cristina Baleeiro Beltrão-Braga, Cristiane Valverde Wenceslau, Leandro Fadel, Daniele dos Santos Martins, Carlos Eduardo Ambrósio, João Flávio Panattoni Martins, and Alexandre Kerkis

Subjects

Pathology, medicine.medical_specialty, Cell type, Transplantation, Heterologous, Biocompatible Materials, Mesenchymal Stem Cell Transplantation, Bone tissue, Random Allocation, Femoral head, Femur Head Necrosis, medicine, Animals, Humans, Bone regeneration, Dental Pulp, Sheep, business.industry, Stem Cells, Mesenchymal stem cell, Femur Head, Surgery, Transplantation, Disease Models, Animal, medicine.anatomical_structure, Hip Joint, Bone marrow, Stem cell, business, OVINOS

Abstract

PURPOSE: Evaluate the bone tissue recovery following transplantation of ovine mesenchymal stem cells (MSC) from bone marrow and human immature dental-pulp stem cells (hIDPSC) in ovine model of induced osteonecrosis of femoral head (ONFH). METHODS: Eight sheep were divided in three experimental groups. First group was composed by four animals with ONFH induced by ethanol through central decompression (CD), for control group without any treatment. The second and third group were compose by two animals, six weeks after ONFH induction received transplantation of heterologous ovine MSC (CD + oMSC), and hIDPSC (CD + hIDPSC), respectively. In both experiments the cells were transplanted without application of any type of immunosupression protocol. RESULTS: Our data indicate that both cell types used in experiments were able to proliferate within injured site providing bone tissue recovery. The histological results obtained from CD+hIDPSC suggested that the bone regeneration in such animals was better than that observed in CD animals. CONCLUSION: Mesenchymal stem cell transplant in induced ovine osteonecrosis of femoral head by central decompression technique is safe, and apparently favors bone regeneration of damaged tissues.

Published

2010

87. Expression of extracellular matrix proteins in human dental pulp stem cells depends on the donor tooth conditions

Author

Sueli Patricia Harumi Miyagi, Manoela Domingues Martins, Márcia Martins Marques, Irina Kerkis, Cícera M. Gomes, and Carlos Magno da Costa Maranduba

Subjects

Male, Pathology, medicine.medical_specialty, Adolescent, Root Resorption, Tenascin, Biology, Collagen Type I, Cell Line, Tooth Eruption, Extracellular matrix, stomatognathic system, Dental pulp stem cells, medicine, Humans, Tooth, Deciduous, Child, General Dentistry, Dental Pulp, Stem cell transplantation for articular cartilage repair, Extracellular Matrix Proteins, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Stem Cells, Tissue Donors, Cell biology, Fibronectins, Fibronectin, Dentition, Permanent, stomatognathic diseases, Microscopy, Fluorescence, Child, Preschool, biology.protein, Female, Stem cell, Type I collagen, Adult stem cell

Abstract

Introduction Stem cells are characterized by the ability to renew themselves through mitotic cell division and differentiating into a diverse range of specialized cell types. An important source of adult stem cells is the dental pulp. In dentistry, regenerative strategies are of importance because of hard dental tissue damage especially as result of caries lesions, trauma, or iatrogenic procedures. The regeneration of dental tissues relies on the ability of stem cells to produce extracellular (ECM) proteins encountered in the dental pulp tissue. Thus, the aim of this study was to analyze the expression and distribution of proteins encountered in dental pulp ECM (type I collagen, fibronectin, and tenascin) in stem cells. Methods Human immature dental pulp stem cells (hIDPSCs) from deciduous (DL-1 and DL-4 cell lines) and permanent (DL-2) teeth were used. The distribution of ECM proteins was observed using the immunofluorescence technique. The gene expression profile was evaluated using reverse transcription polymerase chain reaction (RT-PCR) analysis. Results Positive reactions for all ECM proteins were observed independently of the hIDPSCs analyzed. Type I collagen appeared less evident in DL-2 than in other hIDPSCs. Fibronectin and tenascin were less clear in DL-4. The RT-PCR reactions showed that type I collagen was lesser expressed in the DL-2 cells, whereas fibronectin and tenascin were similarly expressed in all hIDPSCs. Conclusions The distribution and expression of ECM proteins differ among the hIDPSCs. These differences seemed to be related to the donor tooth conditions (deciduous or permanent, retained or erupted, and degree of root reabsorption).

Published

2009

88. Human immature dental pulp stem cells share key characteristic features with limbal stem cells

Author

Gustavo Barreto Melo, Humberto F. Cerruti, Ricardo Luiz Smith, José Álvaro Pereira Gomes, Alexandre Kerkis, Babyla Geraldes Monteiro, R. C. Serafim, Marcelo Cavenaghi Pereira da Silva, Carlos Magno da Costa Maranduba, Irina Kerkis, and Nelson F. Lizier

Subjects

Male, Pathology, medicine.medical_specialty, Vimentin, Cornea, Dental pulp stem cells, Burns, Chemical, medicine, Animals, Humans, Regeneration, Cells, Cultured, Dental Pulp, Corneal epithelium, biology, Stem Cells, Mesenchymal stem cell, Epithelium, Corneal, Cell Differentiation, Cell Biology, General Medicine, Anatomy, Original Articles, Embryonic stem cell, Epithelium, Transplantation, Disease Models, Animal, Eye Burns, medicine.anatomical_structure, biology.protein, sense organs, Rabbits, Stem cell, Biomarkers, Stem Cell Transplantation

Abstract

Objectives: Limbal stem cells (LSC) are self-renewing, highly proliferative cells in vitro, which express a set of specific markers and in vivo have the capacity to reconstruct the entire corneal epithelium in cases of ocular surface injury. Currently, LSC transplantation is a commonly used procedure in patients with either uni- or bilateral total limbal stem cells deficiency (TLSCD). Although LSC transplantation holds great promise for patients, several problems need to be overcome. In order to find an alternative source of cells that can partially substitute LSC in cornea epithelium reconstruction, we aimed at investigating whether human immature dental pulp stem cells (hIDPSC) would present similar key characteristics as LSC and whether they could be used for corneal surface reconstruction in a rabbit TLSCD model. Materials: We used hIDPSC, which co-express mesenchymal and embryonic stem cell markers and present the capacity to differentiate into derivative cells of the three germinal layers. TLSCD was induced by chemical burn in one eye of rabbits. After 30 days, the opaque tissue formed was removed by superficial keratectomy. Experimental group received undifferentiated hIDPSC, while control group only received amniotic membrane (AM). Both groups were sacrificed after 3 months. Results and conclusions: We have demonstrated, using immunohistochemistry and reverse transcription–polymerase chain reaction, that hIDPSCs express markers in common with LSC, such as ABCG2, integrin β1, vimentin, p63, connexin 43 and cytokeratins 3/12. They were also capable of reconstructing the eye surface after induction of unilateral TLSCD in rabbits, as shown by morphological and immunohistochemical analysis using human-specific antibodies against limbal and corneal epithelium. Our data suggest that hIDPSCs share similar characteristics with LSC and might be used as a potential alternative source of cells for corneal reconstruction.

Published

2009

89. Human immature dental pulp stem cells' contribution to developing mouse embryos: production of human/mouse preterm chimaeras

Author

T de Mello Cintra Lavagnolli, Carlos Eduardo Ambrósio, S. A. S. Fonseca, V de Souza Pereira, R. C. Serafim, Maria Angélica Miglino, S. Abdelmassih, C Mota Mendes, Alexandre Kerkis, Irina Kerkis, E J Clemente Santos, José Antonio Visintin, and Roger Abdelmassih

Subjects

Male, Cell type, Mammalian embryology, Embryonic Development, Mice, Inbred Strains, In situ hybridization, Biology, Epithelium, Andrology, Mice, Fetus, Dental pulp stem cells, Inner cell mass, Animals, Humans, Dental Pulp, In Situ Hybridization, Fluorescence, Muscle Cells, Transplantation Chimera, Chromosomes, Human, Y, Muscles, Embryogenesis, Animal Structures, Embryo, Cell Differentiation, Epithelial Cells, Cell Biology, General Medicine, Original Articles, Embryo Transfer, Embryo, Mammalian, Embryo transfer, Adult Stem Cells, Blastocyst, Immunology, embryonic structures, Female

Abstract

Objectives: In this study, we aimed at determining whether human immature dental pulp stem cells (hIDPSC) would be able to contribute to different cell types in mouse blastocysts without damaging them. Also, we analysed whether these blastocysts would progress further into embryogenesis when implanted to the uterus of foster mice, and develop human/mouse chimaera with retention of hIDPSC derivates and their differentiation. Materials and Methods: hIDPSC and mouse blastocysts were used in this study. Fluorescence staining of hIDPSC and injection into mouse blastocysts, was performed. Histology, immunohistochemistry, fluorescence in situ hybridization and confocal microscopy were carried out. Results and Conclusion: hIDPSC showed biological compatibility with the mouse host environment and could survive, proliferate and contribute to the inner cell mass as well as to the trophoblast cell layer after introduction into early mouse embryos (n = 28), which achieved the hatching stage following 24 and 48 h in culture. When transferred to foster mice (n = 5), these blastocysts with hIDPSC (n = 57) yielded embryos (n = 3) and foetuses (n = 6); demonstrating presence of human cells in various organs, such as brain, liver, intestine and hearts, of the human/mouse chimaeras. We verified whether hIDPSC would also be able to differentiate into specific cell types in the mouse environment. Contribution of hIDPSC in at least two types of tissues (muscles and epithelial), was confirmed. We showed that hIDPSC survived, proliferated and differentiated in mouse developing blastocysts and were capable of producing human/mouse chimaeras.

Published

2009

90. Characterization of equine adipose tissue-derived progenitor cells before and after cryopreservation

Author

Alexandre Kerkis, Lisley I. Mambelli, Enrico J.C. Santos, Mariana B. Chaparro, André Luis do Valle de Zoppa, Irina Kerkis, and Paulo Frazão

Subjects

Pathology, medicine.medical_specialty, Biomedical Engineering, Medicine (miscellaneous), Adipose tissue, Bioengineering, Cell Separation, Biology, Cell morphology, Cryopreservation, Extracellular matrix, Osteogenesis, medicine, Animals, Horses, Progenitor cell, Cell Shape, Cell Proliferation, Adipogenesis, Stem Cells, Cell biology, Adipose Tissue, Stem cell, Chondrogenesis, Immunostaining

Abstract

In horses, stem cell therapies are a promising tool to the treatment of many injuries, which are common consequences of athletic endeavor, resulting in high morbidity and often compromising the performance. In spite of many advantages, the isolation of stem cells similar to human, from equine adipose tissue, occurred only recently. The aim of this study was to isolate equine adipose tissue-derived progenitor cells (eAT-PC), to characterize their proliferative potential, and to study their differentiation capacity before and after cryopreservation. The cells, isolated from horse adipose tissue, presented similar fibroblast-like cell morphology in vitro. Their proliferation rate was evaluated during 63 days (23 passages) before and after cryopreservation. After the induction of osteogenic differentiation, von Kossa staining and positive immunostaining studies revealed the formation of calcified extracellular matrix confirming the osteogenic potential of these cells. Adipogenic differentiation was induced using two protocols: routine and other one developed by us, while our protocol requires a shorter time (Oil Red O staining revealed significant accumulation of lipid droplets after 7 days). Chondrogenic differentiation was observed after 21 days of induced pellet culture, as evidenced by histological (toluidine blue) and immunohistochemistry studies. Our data demonstrate that eAT-PC can be easily isolated and successfully expanded in vitro while presenting significant proliferating rate. These cells can be maintained undifferentiated in vitro and can efficiently undergo differentiation at least into mesodermal derivates. These eAT-PC properties were preserved even after cryopreservation. Our findings classify eAT-PC as a promising type of progenitor cells that can be applied in different cell therapies in equines.

Published

2009

91. New source of muscle-derived stem cells with potential for alveolar bone reconstruction in cleft lip and/or palate patients

Author

Felipe T. Salles, Ana de Almeida, Roberto D. Fanganiello, André de Mendonça Costa, Marília Trierveiler Martins, Nivaldo Alonso, Gerson Shigeru Kobayashi, Eder Zucconi, Daniela Franco Bueno, Irina Kerkis, Maria Rita Passos-Bueno, and Cássio Eduardo Raposo do Amaral

Subjects

medicine.medical_specialty, Bone Regeneration, Cleft Lip, Biomedical Engineering, Bioengineering, Cell Separation, Biochemistry, Bone and Bones, Immunophenotyping, Biomaterials, Osteogenesis, Medicine, Animals, Humans, Cell Lineage, Rats, Wistar, Bone regeneration, Dental alveolus, Surgical repair, business.industry, Muscles, Stem Cells, Mesenchymal stem cell, Bone Marrow Stem Cell, Infant, DNA, Fibroblasts, Plastic Surgery Procedures, Flow Cytometry, Surgery, Rats, Cleft Palate, Stem cell, Cheiloplasty, business

Abstract

Cleft lip and palate (CLP), one of the most frequent congenital malformations, affects the alveolar bone in the great majority of the cases, and the reconstruction of this defect still represents a challenge in the rehabilitation of these patients. One of the current most promising strategy to achieve this goal is the use of bone marrow stem cells (BMSC); however, isolation of BMSC or iliac bone, which is still the mostly used graft in the surgical repair of these patients, confers site morbidity to the donor. Therefore, in order to identify a new alternative source of stem cells with osteogenic potential without conferring morbidity to the donor, we have used orbicular oris muscle (OOM) fragments, which are regularly discarded during surgery repair (cheiloplasty) of CLP patients. We obtained cells from OOM fragments of four unrelated CLP patients (CLPMDSC) using previously described preplating technique. These cells, through flow cytometry analysis, were mainly positively marked for five mesenchymal stem cell antigens (CD29, CD90, CD105, SH3, and SH4), while negative for hematopoietic cell markers, CD14, CD34, CD45, and CD117, and for endothelial cell marker, CD31. After induction under appropriate cell culture conditions, these cells were capable to undergo chondrogenic, adipogenic, osteogenic, and skeletal muscle cell differentiation, as evidenced by immunohistochemistry. We also demonstrated that these cells together with a collagen membrane lead to bone tissue reconstruction in a critical-size cranial defects previously induced in nonimmunocompromised rats. The presence of human DNA in the new bone was confirmed by PCR with human-specific primers and immunohistochemistry with human nuclei antibodies. In conclusion, we showed that cells from OOM have phenotypic and behavior characteristics similar to other adult stem cells, both in vitro and in vivo. Our findings suggest that these cells represent a promising source of stem cells for alveolar bone grafting treatment, particularly in young CLP patients.

Published

2008

92. Development of artificial gametes

Author

Zsolt Peter Nagy, Irina Kerkis, and Ching Chien Chang

Subjects

Male, Nuclear Transfer Techniques, Cell division, Somatic cell, Cellular differentiation, Cloning, Organism, Biology, Models, Biological, Oogenesis, medicine, Humans, Spermatogenesis, Gametogenesis, Embryonic Stem Cells, Germ plasm, Genetics, Obstetrics and Gynecology, Cell Differentiation, Spermatozoa, Cell biology, medicine.anatomical_structure, Germ Cells, Reproductive Medicine, Gamete, Female, Germ line development, Developmental Biology, Adult stem cell

Abstract

Virtually all normal cells can reproduce themselves. The germ cells, however, can initiate reproduction of the entire organism. A special sequence of events, meiosis, is responsible for generating mature germ cells bearing a haploid genome. The basic features of meiosis, i.e. two cell divisions with no intervening DNA replication, resulting in a halving of the chromosome complement, are evident throughout evolution. The idea of generating an artificial gamete was recently put forward to provide an ultimate solution for the treatment of infertility. Currently, there are different strategies to create artificial gametes in vitro, such as converting somatic cells from mitotic division to meiotic division directly (somatic cell haploidization), or de-differentiating somatic cells into embryonic stem (ES) cells and re-differentiating ES cells into gametes, or extracting adult stem cells and re-differentiating them into gametes.

Published

2008

93. In vitro differentiation of male mouse embryonic stem cells into both presumptive sperm cells and oocytes

Author

R. C. Serafim, S. A. S. Fonseca, Irina Kerkis, Alexandre Kerkis, S. Abdelmassih, Roger Abdelmassih, and Thais M.C. Lavagnolli

Subjects

Male, Cellular differentiation, Cloning, Organism, Retinoic acid, Tretinoin, Embryoid body, Biology, chemistry.chemical_compound, DAZL, Mice, Animals, Hormone metabolism, Embryonic Stem Cells, In Situ Hybridization, Fluorescence, Microscopy, Confocal, Cell Differentiation, Acrosin, Sperm, Molecular biology, Embryonic stem cell, Spermatozoa, Hormones, Cell biology, Microscopy, Electron, chemistry, Genetic Techniques, Microscopy, Fluorescence, Oocytes, Developmental Biology, Biotechnology

Abstract

Pioneer work in male mouse embryonic stem (ES) cells differentiation into germ cells (GC) showed generations of male or female gametes in separate experiments, using genetically manipulated or preselected ES cells. In an attempt to produce both types of gametes from male mouse ES cells without any genetic manipulation or preselection, we induce the differentiation by retinoic acid (RA) within nonadherent embryoid bodies (EB). It seems that gamete-like cell formation occurs in the correct manner based on the expression of early and late GC-specific genes such as Oct-4, Mvh, Stella, Dazl, Piwil 2, Pdrd 1, Rex 14, Rnf 17, Bmp8b, Acrosin, Stra-8, Haprin, LH-R, Gdf9, Zp3, Zp2, Sycp1, and Sycp3. Immunofluorescence analysis of morphologically well-formed GC and presumptive gametes showed positive labeling for SSEA1, Oct-4, EMA-1, FE-J1, Dazl, Fragilis, Mvh, Acrosin, and acetylated alpha-tubulin. Conventional cytogenetic and FISH analysis indicated a chromosome reduction in ES-derived GC. Our data suggest that ES cells with XY chromosomes can produce under the same experimental conditions both types of presumptive gametes, and this production depends on their positional and temporal information within the EB context.

Published

2007

94. Crotamine mediates gene delivery into cells through the binding to heparan sulfate proteoglycans

Author

Helena B. Nader, Alexandre Kerkis, Ivarne L.S. Tersariol, Vitor Oliveira, Irina Kerkis, Tetsuo Yamane, Gandhi Rádis-Baptista, Eduardo B. Oliveira, Mirian A. F. Hayashi, and Fabio D. Nascimento

Subjects

Endosome, Cell, Genetic Vectors, CHO Cells, Endosomes, Gene delivery, Biology, Endocytosis, Biochemistry, Mice, Cricetulus, Cricetinae, Crotalid Venoms, medicine, Animals, Molecular Biology, Embryonic Stem Cells, Cell Proliferation, Cell growth, Chinese hamster ovary cell, Cell Membrane, Gene Transfer Techniques, Cell Biology, Crotamine, Cytosol, medicine.anatomical_structure, Proteoglycans, Heparan Sulfate Proteoglycans

Abstract

Recently we have shown that crotamine, a toxin from the South American rattlesnake Crotalus durissus terrificus venom, belongs to the family of cell-penetrating peptides. Moreover, crotamine was demonstrated to be a marker of centrioles, of cell cycle, and of actively proliferating cells. Herein we show that this toxin at non-toxic concentrations is also capable of binding electrostatically to plasmid DNA forming DNA-peptide complexes whose stabilities overcome the need for chemical conjugation for carrying nucleic acids into cells. Interestingly, crotamine demonstrates cell specificity and targeted delivery of plasmid DNA into actively proliferating cells both in vitro and in vivo, which distinguishes crotamine from other known natural cell-penetrating peptides. The mechanism of crotamine penetration and cargo delivery into cells was also investigated, showing the involvement of heparan sulfate proteoglycans in the uptake phase, which is followed by endocytosis and peptide accumulation within the acidic endosomal vesicles. Finally, the permeabilization of endosomal membranes induced by crotamine results in the leakage of the vesicles contents to the cell cytosol.

Published

2007

95. Apert p.Ser252Trp Mutation in FGFR2 Alters Osteogenic Potential and Gene Expression of Cranial Periosteal Cells

Author

Roberto D. Fanganiello, Daniela Franco Bueno, Irina Kerkis, Maria Rita Passos-Bueno, Andréa L. Sertié, Sergio Verjovski-Almeida, Sergio Cavalheiro, Renato da Silva Freitas, Nélio A. J. Oliveira, Erika Yeh, Eduardo M. Reis, Nivaldo Alonso, and Hamilton Matsushita

Subjects

Male, Adolescent, Gene Expression, Biology, medicine.disease_cause, Downregulation and upregulation, Osteogenesis, Periosteum, Gene expression, Genetics, medicine, Serine, Humans, Cell Lineage, Receptor, Fibroblast Growth Factor, Type 2, Cell adhesion, Child, Molecular Biology, Gene, Genetics (clinical), Research Articles, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Mutation, Cell growth, Gene Expression Profiling, Skull, Tryptophan, Gene Expression Regulation, Developmental, Infant, Cell Differentiation, Acrocephalosyndactylia, Fibroblasts, Cell biology, Amino Acid Substitution, Child, Preschool, Molecular Medicine, Female, Extracellular matrix organization

Abstract

Apert syndrome (AS), a severe form of craniosynostosis, is caused by dominant gain-of-function mutations in FGFR2. Because the periosteum contribution to AS cranial pathophysiology is unknown, we tested the osteogenic potential of AS periosteal cells (p.Ser252Trp mutation) and observed that these cells are more committed toward the osteoblast lineage. To delineate the gene expression profile involved in this abnormal behavior, we performed a global gene expression analysis of coronal suture periosteal cells from seven AS patients (p.Ser252Trp), and matched controls. We identified 263 genes with significantly altered expression in AS samples (118 upregulated, 145 downregulated; SNRor= |0.4|, Por= 0.05). Several upregulated genes are involved in positive regulation of cell proliferation and nucleotide metabolism, whereas several downregulated genes are involved in inhibition of cell proliferation, gene expression regulation, cell adhesion, and extracellular matrix organization, and in PIK3-MAPK cascades. AS expression profile was confirmed through real-time PCR of a selected set of genes using RNAs from AS and control cells as well as from control cells treated with high FGF2 concentration, and through the analysis of genes involved in FGF-FGFR signaling. Our results allowed us to: (a) suggest that AS periosteal cells present enhanced osteogenic potential, (b) unravel a specific gene expression signature characteristic of AS periosteal cells which may be associated with their osteogenic commitment, (c) identify a set of novel genes involved in the pathophysiology of AS or other craniosynostotic conditions, and (d) suggest for the first time that the periosteum might be involved in the pathophysiology of AS.

Published

2007

96. Isolation and characterization of a population of immature dental pulp stem cells expressing OCT-4 and other embryonic stem cell markers

Author

Gaëlle Chopin Stukart-Parsons, Arnold I. Caplan, D. Dozortsev, Lygia da Veiga Pereira, Humberto F. Cerruti, Alexandre Kerkis, Silvia Maria Gomes Massironi, and Irina Kerkis

Subjects

Histology, medicine.medical_treatment, Cell Culture Techniques, Oct-4, Biology, Dental pulp stem cells, medicine, Humans, Tooth, Deciduous, Child, Dental Pulp, Stem cell transplantation for articular cartilage repair, DNA Primers, Reverse Transcriptase Polymerase Chain Reaction, Stem Cells, Amniotic stem cells, Cell Differentiation, Stem-cell therapy, Immunohistochemistry, Cell biology, Clone Cells, Culture Media, Amniotic epithelial cells, Child, Preschool, Karyotyping, embryonic structures, Anatomy, Stem cell, Octamer Transcription Factor-3, Biomarkers, Cell Division, Adult stem cell

Abstract

We report the isolation of a population of immature dental pulp stem cells (IDPSC), which express embryonic stem cell markers Oct-4, Nanog, SSEA-3, SSEA-4, TRA-1-60 and TRA-1-81 as well as several other mesenchymal stem cell markers during at least 25 passages while maintaining the normal karyotype and the rate of expansion characteristic of stem cells. The expression of these markers was maintained in subclones obtained from these cells. Moreover, in vitrothese cells can be induced to undergo uniform differentiation into smooth and skeletal muscles, neurons, cartilage, and bone under chemically defined culture conditions. After in vivo transplantation of these cells into immunocompromised mice, they showed dense engraftment in various tissues. The relative ease of recovery and the expression profiles of various markers justify further exploration of IDPSC for clinical therapy.

Published

2006

97. Properties of cell penetrating peptides (CPPs)

Author

Mirian A. F. Hayashi, Irina Kerkis, Alexandre Kerkis, and Tetsuo Yamane

Subjects

Genetic enhancement, Clinical Biochemistry, Cell, Intracellular Space, Biology, Biochemistry, Viral vector, chemistry.chemical_compound, Drug Delivery Systems, Genetics, medicine, Humans, Enhancer, Cytoskeleton, Molecular Biology, Gene, Cell Proliferation, Cell Membrane, Cell Biology, Molecular biology, Cell biology, Protein Transport, medicine.anatomical_structure, chemistry, Peptides, DNA, Intracellular

Abstract

Different approaches have been developed for the introduction of macromolecules, proteins and DNA into target cells. Viral (retroviruses, lentiviruses, etc.) and nonviral (liposomes, bioballistics etc.) vectors as well as lipid particles have been tested as DNA delivery systems. However, all of them share several undesirable effects that are difficult to overcome, such as unwanted immunoresponse and limited cell targeting. The discovery of the cell penetrating peptides (CPPs) showing properties of macromolecules carriers and enhancers of viral vectors, opened new opportunities for the delivery of biologically active cargos, including therapeutically relevant genes into various cells and tissues. This review summarizes recent data about the best characterized CPPs as well as those sharing cell-penetrating and cargo delivery properties despite differing in the primary sequence. The putative mechanisms of CPPs penetration into cells and interaction with intracellular structures such as chromosomes, cytoskeleton and centrioles are addressed. We further discuss recent developments in overcoming the lack of cells specificity, one of the main obstacles for CPPs application in gene therapy. In particular, we review a newly discovered affinity of CPPs to actively proliferating cells.

Published

2006

98. Establishment of new murine embryonic stem cell lines for the generation of mouse models of human genetic diseases

Author

Lygia da Veiga Pereira, Irina Kerkis, Alexandre Kerkis, Marco Roberto Bourg de Mello, Marina Sukoyan, and José Antonio Visintin

Subjects

Genetically modified mouse, Male, Human genetic diseases, Physiology, Cellular differentiation, Immunology, Biophysics, Mice, Transgenic, Embryoid body, Biology, Biochemistry, Cell Line, Mouse model, Chimera (genetics), Mice, Transgenic mouse, Inner cell mass, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, lcsh:QH301-705.5, Genetics, lcsh:R5-920, Chimera, General Neuroscience, Stem Cells, Totipotent, Genetic Diseases, Inborn, Cell Differentiation, Cell Biology, General Medicine, Alkaline Phosphatase, Embryo, Mammalian, Embryonic stem cell, Cell biology, Disease Models, Animal, Germ Cells, Murine embryonic stem cells, lcsh:Biology (General), Cell culture, Female, lcsh:Medicine (General)

Abstract

Embryonic stem cells are totipotent cells derived from the inner cell mass of blastocysts. Recently, the development of appropriate culture conditions for the differentiation of these cells into specific cell types has permitted their use as potential therapeutic agents for several diseases. In addition, manipulation of their genome in vitro allows the creation of animal models of human genetic diseases and for the study of gene function in vivo. We report the establishment of new lines of murine embryonic stem cells from preimplantation stage embryos of 129/Sv mice. Most of these cells had a normal karyotype and an XY sex chromosome composition. The pluripotent properties of the cell lines obtained were analyzed on the basis of their alkaline phosphatase activity and their capacity to form complex embryoid bodies with rhythmically contracting cardiomyocytes. Two lines, USP-1 and USP-3, with the best in vitro characteristics of pluripotency were used in chimera-generating experiments. The capacity to contribute to the germ line was demonstrated by the USP-1 cell line. This cell line is currently being used to generate mouse models of human diseases.

Published

2002

99. Changes in Expression Pattern of Selected Endometrial Proteins following Mesenchymal Stem Cells Infusion in Mares with Endometrosis

Author

Gustavo Henrique Zimmermann Winter, Bruna P. Morais, Lisley I. Mambelli, Maria Angélica Miglino, Eduardo Malschitzky, Dener S. Madeiro, Rodrigo Costa Mattos, Irina Kerkis, and Alexandre Kerkis

Subjects

Proteomics, Pathology, Biopsy, Cellular differentiation, lcsh:Medicine, Adipose tissue, Vimentin, Biochemistry, Endometrium, Animal Cells, lcsh:Science, TECIDO ADIPOSO, Endometrosis, Multidisciplinary, Stem Cells, Animal Models, Veterinary Diseases, Female, Cellular Types, Immunohistochemical Analysis, Veterinary Pathology, Research Article, Veterinary Medicine, medicine.medical_specialty, Stromal cell, Immunology, Endometriosis, Biology, Mesenchymal Stem Cell Transplantation, Research and Analysis Methods, Cytokeratin, Model Organisms, medicine, Animals, Horses, Immunohistochemistry Techniques, Mucous Membrane, Gene Expression Profiling, lcsh:R, Mesenchymal stem cell, Biology and Life Sciences, Mesenchymal Stem Cells, Cell Biology, Histochemistry and Cytochemistry Techniques, Transplantation, Immunologic Techniques, biology.protein, Veterinary Science, lcsh:Q, Transcriptome, Biomarkers, Protein Abundance, Developmental Biology

Abstract

Mesenchymal stem cells (MSCs) due to their self-renewal potential and differentiation capacity are useful for tissue regeneration. Immunomodulatory and trophic properties of MSCs were demonstrated suggesting their use as medicinal signaling cells able to positively change local environment in injured tissue. Equine endometrosis is a progressive degenerative disease responsible for glandular alterations and endometrial fibrosis which causes infertility in mares. More precisely, this disease is characterized by phenotypic changes in the expression pattern of selected endometrial proteins. Currently, no effective treatment is available for endometrosis. Herein, we aimed at the evaluation of expression pattern of these proteins after allogeneic equine adipose tissue-derived multipotent mesenchymal stem cells (eAT-MSCs) infusion as well as at testing the capacity of these cells to promote endometrial tissue remodeling in mares with endometrosis. eAT-MSC (2 × 10(7)/animal) were transplanted into mares' uterus and control animals received only placebo. Uterine biopsies were collected before (day 0) and after (days 7, 21 and 60) cells transplantation. Conventional histopathology as well as expression analysis of such proteins as laminin, vimentin, Ki-67-antigen, α-smooth muscle actin (α-SMA) and cytokeratin 18 (CK18) have been performed before and after eAT-MSCs transplantation. We demonstrated that eAT-MSCs induced early (at day 7) remodeling of endometrial tissue microenvironment through changes observed in intra cellular and intra glandular localization of aforementioned proteins. We demonstrated that eAT-MSCs were able to positively modulate the expression pattern of studied secretory proteins as well as, to promote the induction of glandular epithelial cells proliferation suggesting local benefits to committed endometrial tissue environment after eAT-MSCs transplantation.

Published

2014

100. Pluripotent Stem Cells as an In Vitro Model of Neuronal Differentiation

Author

Irina Kerkis, Mirian A. F. Hayashi, Nelson F. Lizier, Antonio C. Cassola, Lygia V. Pereira, Alexandre Kerkis, Irina Kerkis, Mirian A. F. Hayashi, Nelson F. Lizier, Antonio C. Cassola, Lygia V. Pereira, and Alexandre Kerkis

Published

2011