Your search keyword '"Tarantal, Alice F."' showing total 60 results

1. Systemic and Persistent Muscle Gene Expression in Rhesus Monkeys with a Liver De-Targeted Adeno-Associated Virus Vector.

Author

Tarantal, Alice F., Lee, C. Chang I., Martinez, Michele L., Asokan, Aravind, and Samulski, R.Jude

Subjects

*TRANSGENE expression, *MUSCULOSKELETAL system diseases, *HEART diseases, *ADENO-associated virus, *RHESUS monkeys, *LUCIFERASES, *DISEASES

Abstract

The liver is a major off-target organ in gene therapy approaches for cardiac and musculoskeletal disorders. Intravenous administration of most of the naturally occurring adeno-associated virus (AAV) strains invariably results in vector genome sequestration within the liver. In the current study, we compared the muscle tropism and transduction efficiency of a liver de-targeted AAV variant to AAV9 following systemic administration in newborn rhesus monkeys. In vivo bioluminescence imaging was performed to monitor transgene expression (firefly luciferase) post administration. Results indicated comparable and sustained levels of systemic firefly luciferase gene expression in skeletal muscle over a period of two years. Quantitation of vector biodistribution in harvested tissues post-administration revealed widespread recovery of vector genomes delivered by AAV9 but markedly decreased levels in major systemic organs from the AAV variant. These studies validate the translational potential and safety of liver de-targeted AAV strains for gene therapy of muscle-related diseases. [ABSTRACT FROM AUTHOR]

Published

2017

2. Clonidine inhibits anti-non-Gal IgM xenoantibody elicited in multiple pig-to-primate models.

Author

Stewart, John M., Tarantal, Alice F., Hawthorne, Wayne J., Salvaris, Evelyn J., O'Connell, Philip J., Nottle, Mark B., d'Apice, Anthony J. F., Cowan, Peter J., and Kearns‐Jonker, Mary

Abstract

Background: Survival of vascularized xenografts is dependent on pre-emptive inhibition of the xenoantibody response against galactosyltransferase knockout (GTKO) porcine organs. Our analysis in multiple GTKO pig-to-primate models of xenotransplantation has demonstrated that the anti-non-gal-α-1,3-gal (anti-non-Gal) xenoantibody response displays limited structural diversity. This allowed our group to identify an experimental compound which selectively inhibited induced anti-non-Gal IgM xenoantibodies. However, because this compound had an unknown safety profile, we extended this line of research to include screening small molecules with known safety profiles allowing rapid advancement to large animal models. Methods: The NIH clinical collections of small molecules were screened by ELISA for their ability to inhibit xenoantibody binding to GTKO pig endothelial cells. Serum collected from non-immuno-suppressed rhesus monkeys at day 14 post-injection with GTKO pig endothelial cells was utilized as a source of elicited xenoantibody for initial screening. Virtual small molecule screening based on xenoantibody structure was used to assess the likelihood that the identified small molecules bound xenoantibody directly. As a proxy for selectivity, ELISAs against tetanus toxoid and the natural antigens laminin, thyroglobulin, and single-stranded DNA (ssDNA) were utilized to assess the ability of the identified reagents to inhibit additional antibody responses. The identified inhibitory small molecules were further tested for their ability to inhibit xenoantibody elicited in multiple settings, including rhesus monkeys pre-treated with an anti-non-Gal selective anti-idiotypic antibody, non-immunosuppressed rhesus monkeys immunized with wild-type fetal pig isletlike cell clusters, and non-immunosuppressed baboons transplanted with GTKO multiple transgenic pig kidneys. Results: Four clinically relevant small molecules inhibited anti-non-Gal IgM binding to GTKO pig endothelial cells in vitro. Three of these drugs displayed a limited region of structural similarity suggesting they may inhibit xenoantibody by a similar mechanism. One of these, the anti-hypertensive agent clonidine, displayed only minimal inhibition of antibodies elicited by vaccination against tetanus toxoid or pre-existing natural antibodies against laminin, thyroglobulin, or ssDNA. Furthermore, clonidine inhibited elicited anti-non-Gal IgM from all animals that demonstrated a xenoantibody response in each experimental setting. Conclusions: Clinically relevant small molecule drugs with known safety profiles can inhibit xenoantibody elicited against non-Gal antigens in diverse experimental xenotransplantation settings. These molecules are ready to be tested in large animal models. However, it will first be necessary to optimize the timing and dosing required to inhibit xenoantibodies in vivo. [ABSTRACT FROM AUTHOR]

Published

2015

3. Effects of Vector Backbone and Pseudotype on Lentiviral Vector-mediated Gene Transfer: Studies in Infant ADA-Deficient Mice and Rhesus Monkeys.

Author

Carbonaro Sarracino, Denise, Tarantal, Alice F, Lee, C Chang I., Martinez, Michele, Jin, Xiangyang, Wang, Xiaoyan, Hardee, Cinnamon L, Geiger, Sabine, Kahl, Christoph A, and Kohn, Donald B

Subjects

*GENETIC transformation, *ADENOSINE deaminase deficiency, *ANTISENSE DNA, *LABORATORY mice, *RHESUS monkeys

Abstract

Systemic delivery of a lentiviral vector carrying a therapeutic gene represents a new treatment for monogenic disease. Previously, we have shown that transfer of the adenosine deaminase (ADA) cDNA in vivo rescues the lethal phenotype and reconstitutes immune function in ADA-deficient mice. In order to translate this approach to ADA-deficient severe combined immune deficiency patients, neonatal ADA-deficient mice and newborn rhesus monkeys were treated with species-matched and mismatched vectors and pseudotypes. We compared gene delivery by the HIV-1-based vector to murine γ-retroviral vectors pseudotyped with vesicular stomatitis virus-glycoprotein or murine retroviral envelopes in ADA-deficient mice. The vesicular stomatitis virus-glycoprotein pseudotyped lentiviral vectors had the highest titer and resulted in the highest vector copy number in multiple tissues, particularly liver and lung. In monkeys, HIV-1 or simian immunodeficiency virus vectors resulted in similar biodistribution in most tissues including bone marrow, spleen, liver, and lung. Simian immunodeficiency virus pseudotyped with the gibbon ape leukemia virus envelope produced 10- to 30-fold lower titers than the vesicular stomatitis virus-glycoprotein pseudotype, but had a similar tissue biodistribution and similar copy number in blood cells. The relative copy numbers achieved in mice and monkeys were similar when adjusted to the administered dose per kg. These results suggest that this approach can be scaled-up to clinical levels for treatment of ADA-deficient severe combined immune deficiency subjects with suboptimal hematopoietic stem cell transplantation options. [ABSTRACT FROM AUTHOR]

Published

2014

4. Rhesus monkeys and baboons develop clotting factor VIII inhibitors in response to porcine endothelial cells or islets.

Author

Stewart, John M., Tarantal, Alice F., Hawthorne, Wayne J., Salvaris, Evelyn J., O'Connell, Philip J., Nottle, Mark B., d'Apice, Anthony J. F., Cowan, Peter J., and Kearns‐Jonker, Mary

Subjects

*XENOTRANSPLANTATION, *ORGAN donors, *HEMOSTATICS, *TRANSGENIC animals, *ISLANDS of Langerhans, *CHROMOGENIC compounds

Abstract

Background Xenotransplantation of porcine organs holds promise of solving the human organ donor shortage. The use of α-1,3-galactosyltransferase knockout (GTKO) pig donors mitigates hyperacute rejection, while delayed rejection is currently precipitated by potent immune and hemostatic complications. Previous analysis by our laboratory suggests that clotting factor VIII (FVIII) inhibitors might be elicited by the structurally restricted xenoantibody response which occurs after transplantation of either pig GTKO/ hCD55/ hCD59/ hHT transgenic neonatal islet cell clusters or GTKO endothelial cells. Methods A recombinant xenoantibody was generated using sequences from baboons demonstrating an active xenoantibody response at day 28 after GTKO/ hCD55/ hCD59/ hHT transgenic pig neonatal islet cell cluster transplantation. Rhesus monkeys were immunized with GTKO pig endothelial cells to stimulate an anti-non-Gal xenoantibody response. Serum was collected at days 0 and 7 after immunization. A two-stage chromogenic assay was used to measure FVIII cofactor activity and identify antibodies which inhibit FVIII function. Molecular modeling and molecular dynamics simulations were used to predict antibody structure and the residues which contribute to antibody-FVIII interactions. Competition ELISA was used to verify predictions at the domain structural level. Results Antibodies that inhibit recombinant human FVIII function are elicited after non-human primates are transplanted with either GTKO pig neonatal islet cell clusters or endothelial cells. There is an apparent increase in inhibitor titer by 15 Bethesda units (Bu) after transplant, where an increase greater than 5 Bu can indicate pathology in humans. Furthermore, competition ELISA verifies the computer modeled prediction that the recombinant xenoantibody, H66K12, binds the C1 domain of FVIII. Conclusions The development of FVIII inhibitors is a novel illustration of the potential impact the humoral immune response can have on coagulative dysfunction in xenotransplantation. However, the contribution of these antibodies to rejection pathology requires further evaluation because 'normal' coagulation parameters after successful xenotransplantation are not fully understood. [ABSTRACT FROM AUTHOR]

Published

2014

5. Anti-non- Gal-specific combination treatment with an anti-idiotypic Ab and an inhibitory small molecule mitigates the xenoantibody response.

Author

Stewart, John M., Tarantal, Alice F., Chen, Yan, Appleby, Nancy C., Fuentes, Tania I., Lee, C. Chang I., Salvaris, Evelyn J., d'Apice, Anthony J. F., Cowan, Peter J., and Kearns‐Jonker, Mary

Subjects

*GALACTOSYLTRANSFERASE genetics, *SELECTIVE inhibition (Chemistry), *XENOGRAFTS, *ANTI-idiotypic antibodies, *SMALL molecules

Abstract

Background B-cell depletion significantly extends survival of α-1,3-galactosyltranferase knockout ( GTKO) porcine organs in pig-to-primate models. Our previous work demonstrated that the anti-non-Gal xenoantibody response is structurally restricted. Selective inhibition of xenoantigen/xenoantibody interactions could prolong xenograft survival while preserving B-cell-mediated immune surveillance. Methods The anti-idiotypic antibody, B4N190, was selected from a synthetic human phage display library after enrichment against a recombinant anti-non-Gal xenoantibody followed by functional testing in vitro. The inhibitory small molecule, JMS022, was selected from the NCI diversity set III using virtual screening based on predicted xenoantibody structure. Three rhesus monkeys were pre-treated with anti-non-Gal-specific single-chain anti-idiotypic antibody, B4N190. A total of five monkeys, including two untreated controls, were then immunized with GTKO porcine endothelial cells to initiate an anti-non-α-1,3-Gal (non-Gal) xenoantibody response. The efficacy of the inhibitory small molecule specific for anti-non-Gal xenoantibody, JMS022, was tested in vitro. Results After the combination of in vivo anti-id and in vitro small molecule treatments, IgM xenoantibody binding to GTKO cells was reduced to pre-immunization levels in two-thirds of animals; however, some xenoantibodies remained in the third animal. Furthermore, when treated with anti-id alone, all three experimental animals displayed a lower anti-non-Gal IgG xenoantibody response compared with controls. Treatment with anti-idiotypic antibody alone reduced IgM xenoantibody response intensity in only one of three monkeys injected with GTKO pig endothelial cells. In the one experimental animal, which displayed reduced IgM and IgG responses, select B-cell subsets were also reduced by anti-id therapy alone. Furthermore, natural antibody responses, including anti-laminin, anti-ss DNA, and anti-thyroglobulin antibodies were intact despite targeted depletion of anti-non-Gal xenoantibodies in vivo indicating that selective reduction of xenoantibodies can be accomplished without total B-cell depletion. Conclusions This preliminary study demonstrates the strength of approaches designed to selectively inhibit anti-non-Gal xenoantibody. Both anti-non-Gal-specific anti-idiotypic antibody and small molecules can be used to selectively limit xenoantibody responses. [ABSTRACT FROM AUTHOR]

Published

2014

6. Fetal Surgery in the Primate 4.0: A New Technique 30 Years Later.

Author

Perrone, Erin E., Galganski, Laura A., Tarantal, Alice F., Olstad, Katie J., Treadwell, Marjorie C., Berman, Deborah R., Jarboe, Marcus D., Mychaliska, George B., Farmer, Diana L., Perrone, Erin E, Galganski, Laura A, Tarantal, Alice F, Olstad, Katie J, Treadwell, Marjorie C, Berman, Deborah R, Jarboe, Marcus D, Mychaliska, George B, and Farmer, Diana L

Subjects

*FETAL surgery, *RHESUS monkeys, *AMNIOTIC liquid, *MEMBRANE separation, *PRIMATES, *HEALING, *OBSTETRICS surgery, *FETAL diseases, *UTERUS, *PSYCHOLOGICAL tests, *RESEARCH funding, *ANIMALS

Abstract

Introduction: Open fetal surgery requires a hemostatic hysterotomy that minimizes membrane separation. For over 30 years, the standard of care for hysterotomy in the gravid uterus has been the AutoSuture Premium Poly CS*-57 stapler.Objective: In this study, we sought to test the feasibility of hysterotomy in a rhesus monkey model with the Harmonic ACE®+7 Shears.Methods: A gravid rhesus monkey underwent midgestation hysterotomy at approximately 90 days of gestation (2nd trimester; term = 165 ± 10 days) using the Harmonic ACE®+7 Shears. A two-layer uterine closure was completed and the dam was monitored by ultrasound intermittently throughout the pregnancy. At 58 days after hysterotomy (near term), a final surgery was performed to evaluate the uterus and hysterotomy site.Results: A 3.5-cm hysterotomy was completed in 2 min 7 s. The opening was hemostatic and the membranes were sealed. Immediately after closure and throughout the pregnancy, ultrasound revealed intact membranes without separation and normal amniotic fluid levels. At term, the scar was well healed without signs of thinning or dehiscence.Conclusions: The Harmonic ACE®+7 Shears produced a hemostatic midgestation hysterotomy with membrane sealing in the rhesus monkey model. Importantly, healing was acceptable. [ABSTRACT FROM AUTHOR]

Published

2021

7. In Vivo Imaging and Gene Therapy: Monitoring Safety, Biodistribution, and Long-Term Expression with Positron Emission Tomography.

Author

Tarantal, Alice F.

Subjects

*POSITRON emission tomography, *GENE therapy, *GENETIC vectors

Abstract

Significant advancements have been made in the use of noninvasive imaging technologies I in vivo i with direct relevance to the gene therapy field. It should be noted that current conventional PET imaging systems scan a small anatomic area in a single bed position and require a relatively high injected radiotracer dose and extended imaging times to achieve adequate signal-to-noise in the images. Total-body PET and highly stable chelators together enable meaningful 89Zr-antibody-PET studies up to 30 days post-injection. [Extracted from the article]

Published

2020

8. Radiolabeling Human Peripheral Blood Stem Cells for Positron Emission Tomography (PET) Imaging in Young Rhesus Monkeys.

Author

Tarantal, Alice F., Lee, C. Chang I., Kukis, David L., and Cherry, Simon R.

Subjects

*RADIOLABELING, *STEM cells, *POSITRON emission tomography, *COPPER, *ZIRCONIUM, *CD45 antigen, *ANTIBODY-toxin conjugates

Abstract

These studies focused on a new radiolabeling technique with copper (64Cu) and zirconium (89Zr) for positron emission tomography (PET) imaging using a CD45 antibody. Synthesis of 64Cu-CD45 and 89Zr-CD45 immunoconjugates was performed and the evaluation of the potential toxicity of radiolabeling human peripheral blood stem cells (hPBSC) was assessed in vitro (viability, population doubling times, colony forming units). hPBSC viability was maintained as the dose of 64Cu-TETA-CD45 increased from 0 (92%) to 160 µCi/mL (76%, p>0.05). Radiolabeling efficiency was not significantly increased with concentrations of 64Cu-TETA-CD45 >20 µCi/mL (p>0.50). Toxicity affecting both growth and colony formation was observed with hPBSC radiolabeled with ≥40 µCi/mL (p<0.05). For 89Zr, there were no significant differences in viability (p>0.05), and a trend towards increased radiolabeling efficiency was noted as the dose of 89Zr-Df-CD45 increased, with a greater level of radiolabeling with 160 µCi/mL compared to 0–40 µCi/mL (p<0.05). A greater than 2,000 fold-increase in the level of 89Zr-Df-CD45 labeling efficiency was observed when compared to 64Cu-TETA-CD45. Similar to 64Cu-TETA-CD45, toxicity was noted when hPBSC were radiolabeled with ≥40 µCi/mL (p<0.05) (growth, colony formation). Taken together, 20 µCi/mL resulted in the highest level of radiolabeling efficiency without altering cell function. Young rhesus monkeys that had been transplanted prenatally with 25×106 hPBSC expressing firefly luciferase were assessed with bioluminescence imaging (BLI), then 0.3 mCi of 89Zr-Df-CD45, which showed the best radiolabeling efficiency, was injected intravenously for PET imaging. Results suggest that 89Zr-Df-CD45 was able to identify engrafted hPBSC in the same locations identified by BLI, although the background was high. [ABSTRACT FROM AUTHOR]

Published

2013

9. Center for Fetal Monkey Gene Transfer for Heart, Lung, and Blood Diseases: An NHLBI Resource for the Gene Therapy Community.

Author

Tarantal, Alice F. and Skarlatos, Sonia I.

Subjects

*GENETIC transformation, *HEART diseases, *LUNG diseases, *BLOOD diseases, *GENE therapy, *LABORATORY monkeys

Abstract

AbstractThe goals of the National Heart, Lung, and Blood Institute (NHLBI) Center for Fetal Monkey Gene Transfer for Heart, Lung, and Blood Diseases are to conduct gene transfer studies in monkeys to evaluate safety and efficiency; and to provide NHLBI-supported investigators with expertise, resources, and services to actively pursue gene transfer approaches in monkeys in their research programs. NHLBI-supported projects span investigators throughout the United States and have addressed novel approaches to gene delivery; “proof-of-principle”; assessed whether findings in small-animal models could be demonstrated in a primate species; or were conducted to enable new grant or IND submissions. The Center for Fetal Monkey Gene Transfer for Heart, Lung, and Blood Diseases successfully aids the gene therapy community in addressing regulatory barriers, and serves as an effective vehicle for advancing the field. [ABSTRACT FROM AUTHOR]

Published

2012

10. Nonmyeloablative Conditioning Regimen to Increase Engraftment of Gene-modified Hematopoietic Stem Cells in Young Rhesus Monkeys.

Author

Tarantal, Alice F, Giannoni, Francesca, I Lee, C Chang, Wherley, Jennifer, Sumiyoshi, Teiko, Martinez, Michele, Kahl, Christoph A, Elashoff, David, Louie, Stan G, and Kohn, Donald B

Subjects

*IMMUNE response, *TRANSGENES, *GENE therapy, *HEMATOPOIETIC stem cell transplantation, *FLUDARABINE, *SIMIAN immunodeficiency virus, *GREEN fluorescent protein, *THERAPEUTICS

Abstract

Immune responses to transgene products may lead to rejection of transduced cells, limiting successful gene therapy for genetic diseases. While moderate dosages of chemotherapeutic agents such as busulfan may increase hematopoietic stem cells (HSC) engraftment, they are not immune suppressive and do not abrogate immune responses to transgene products. Studies focused on nonmyeloablative conditioning with busulfan ± fludarabine in a clinically relevant monkey model to induce immune suppression to allow cells expressing a foreign transgene product to persist. Bone marrow CD34+ HSC were transduced in two equal fractions using simian immunodeficiency virus (SIV)-based lentiviral vectors carrying a nonexpressed DNA sequence tag (NoN) and the green fluorescent protein (GFP) reporter gene. Post-transplant there was no evidence of elimination of cells containing the potentially immunogenic GFP gene; several recipients had stable persistence of cells, and no differences were detected with fludarabine, which was rapidly cleared. Antibodies and cellular immune responses to GFP developed in recipients with the highest levels of GFP-marked cells, although these cells were not eliminated. These studies establish a clinically relevant pediatric primate model to assess the effects of conditioning regimens on the engraftment of transduced HSC and the immune responses to cells expressing a foreign gene product. [ABSTRACT FROM AUTHOR]

Published

2012

11. Fetal, infant, adolescent and adult phenotypes of polycystic ovary syndrome in prenatally androgenized female rhesus monkeys.

Author

ABBOTT, DAVID H., TARANTAL, ALICE F., and DUMESIC, DANIEL A.

Subjects

*POLYCYSTIC ovary syndrome, *RHESUS monkeys, *FETUS, *ANDROGENS, *METABOLISM

Abstract

Old World monkeys provide naturally occurring and experimentally induced phenotypes closely resembling the highly prevalent polycystic ovary syndrome (PCOS) in women. In particular, experimentally induced fetal androgen excess in female rhesus monkeys produces a comprehensive adult PCOS-like phenotype that includes both reproductive and metabolic dysfunction found in PCOS women. Such a reliable experimental approach enables the use of the prenatally androgenized (PA) female rhesus monkey model to (1) examine fetal, infant and adolescent antecedents of adult pathophysiology, gaining valuable insight into early phenotypic expression of PCOS, and (2) to understand adult pathophysiology from a mechanistic perspective. Elevated circulating luteinizing hormone (LH) levels are the earliest indication of reproductive dysfunction in late gestation nonhuman primate fetuses and infants exposed to androgen excess during early (late first to second trimester) gestation. Such early gestation-exposed PA infants also are hyperandrogenic, with both LH hypersecretion and hyperandrogenism persisting in early gestation-exposed PA adults. Similarly, subtle metabolic abnormalities appearing in young nonhuman primate infants and adolescents precede the abdominal adiposity, hyperliplidemia and increased incidence of type 2 diabetes that characterize early gestation-exposed PA adults. These new insights into the developmental origins of PCOS, and progression of the pathophysiology from infancy to adulthood, provide opportunities for clinical intervention to ameliorate the PCOS phenotype thus providing a preventive health-care approach to PCOS-related abnormalities. For example, PCOS-like traits in PA monkeys, as in PCOS women, can improve with better insulin–glucose homeostasis, suggesting that lifestyle interventions preventing increased adiposity in adolescent daughters of PCOS mothers also may reduce their risk of acquiring many PCOS-related metabolic abnormalities in adulthood. Am. J. Primatol. 71:776–784, 2009. © 2009 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

12. Effects of busulfan dose escalation on engraftment of infant rhesus monkey hematopoietic stem cells after gene marking by a lentiviral vector

Author

Kahl, Christoph A., Tarantal, Alice F., Lee, Chang I., Jimenez, Daniel F., Choi, Christopher, Pepper, Karen, Petersen, Denise, Fletcher, Misty D., Leapley, Alyssa C., Fisher, Jennifer, Burns, Travis S., Ultsch, Man-Ni, Dorey, Frederick J., and Kohn, Donald B.

Subjects

*HEMATOPOIETIC stem cells, *BLOOD cells, *BONE marrow cells, *HEMATOPOIETIC system

Abstract

Objective: Nonmyeloablative cytoreduction is used in clinical hematopoietic stem cell gene therapy trials to increase engraftment of gene-modified cells. We utilized an infant rhesus monkey model to identify an optimal dosage of busulfan that results in efficient long-term gene marking with minimal toxicities. Methods: Bone marrow (BM) was harvested, followed by a single 2-hour intravenous infusion of busulfan at escalating dosages of 0 to 160 mg/m2. CD34+ cells were immunoselected from BM, transduced overnight with a simian immunodeficiency virus–based lentiviral vector carrying a nonexpressed marker gene, and injected intravenously 48 hours post–busulfan administration. Pharmacokinetics were assessed, as well as adverse effects and peripheral blood and BM gene marking. Results: Increasing dosages of busulfan resulted in increased area-under-the-curve (AUC) with some variability at each dosage level, suggesting interindividual variation in clearance. Blood chemistries were normal and no adverse effects were observed as a result of busulfan infusion. At 120 and 160 mg/m2, transient neutropenia and thrombocytopenia were noted but not lymphopenia. Over the 6 months of study posttransplantation, a busulfan dosage-related increase in gene marking was observed ranging from undetectable (no busulfan) up to 0.1% gene-containing cells in animals achieving the highest busulfan AUC. This corresponds to a more than 100-fold increase in gene marking over the busulfan dosage range studied. Conclusions: These data indicate that increased gene marking of hematopoietic stem cells can be achieved by escalating busulfan dosages from 40 to 160 mg/m2 without significant toxicity in infant nonhuman primates. [Copyright &y& Elsevier]

Published

2006

13. Intrapulmonary and intramyocardial gene transfer in rhesus monkeys (Macaca mulatta): Safety and efficiency of HIV-1-derived lentiviral vectors for fetal gene delivery

Author

Tarantal, Alice F., McDonald, Ruth J., Jimenez, Daniel F., Lee, C. Chang I., O’Shea, Cristin E., Leapley, Alyssa C., Won, Rosa H., Plopper, Charles G., Lutzko, Carolyn, and Kohn, Donald B.

Subjects

*GENETIC transformation, *RHESUS monkeys, *CARDIAC imaging, *INTERNAL medicine

Abstract

Abstract: Fetal gene transfer was studied using intrapulmonary and intramyocardial transfer of SIN HIV-1-derived lentiviral vectors expressing EGFP in rhesus monkeys. Fetuses were monitored sonographically during gestation and tissue analyses performed at term or 3 months postnatal age. Animals remained healthy during the study period as evidenced by normal growth, development, hematology, clinical chemistry, echocardiography, and pulmonary function tests. Strong pulmonary fluorescence was observed postnatally after fetal intrapulmonary delivery of lenti-CMV, but not lenti-SP-C, and compared to nontransferred controls. High EGFP copy numbers were found by quantitative PCR with both vector constructs in lung lobes (≤15%) and EGFP copies were also detected in the diaphragm, pericardium, and thorax. No differences were found in lung:body weight ratios, percentage lung parenchyma, or overall morphology when compared to controls. For intramyocardial gene delivery, strong transgene expression was found within the myocardium and pericardium, and high EGFP copy numbers were found by quantitative PCR (3–36%). EGFP was also detected in the aorta, thorax, and diaphragm. These studies indicate that postnatal heart and lung development and function were not altered after fetal intraorgan gene transfer and subsequent transgene expression prenatally and postnatally, and gene transfer was restricted to the thoracic cavity with intrapulmonary and intramyocardial lentiviral vector-mediated gene delivery. [Copyright &y& Elsevier]

Published

2005

14. Fetal and Infant Head Circumference Sexual Dimorphism in Primates.

Author

Joffe, Tracey H., Tarantal, Alice F., Rice, Karen, Leland, Michelle, Oerke, Ann-Kathrin, Rodeck, Charles, Geary, Michael, Hindmarsh, Peter, Wells, Jonathan C. K., and Aiello, Leslie C.

Subjects

*PRIMATES, *DIMORPHISM in animals, *ANIMAL morphology, *BODY size, *ULTRASONIC imaging, *ANTHROPOMETRY, *PHYSICAL anthropology

Abstract

Studies have shown that after controlling for the effects of body size on brain size, the brains of adult humans, rhesus monkeys, and chimpanzees differ in relative size, where males have a greater volume of cerebral tissue than females. We assess whether head circumference sexual dimorphism is present during early development by evaluating sex differences in relative head circumference in living fetuses and infants within the first year of life. Head circumference is used as a proxy for brain size in the fetus and infant. Femur length is used as a proxy for body length in the fetus. Ultrasonography was used to obtain fetal measures, and anthropometry was used to obtain postnatal measures in humans, rhesus monkeys, baboons, and common marmosets. We show that statistically significant but low levels of head circumference sexual dimorphism are present in humans, rhesus monkeys, and baboons in early life. On average, males have head circumferences about 2% larger than females of comparable femur/body length in humans, rhesus monkeys, and baboons. No evidence for head circumference sexual dimorphism in the common marmoset was found. Dimorphism was present across all body size ranges. We suggest that head circumference sexual dimorphism emerges largely postnatally and increases throughout maturation, particularly in humans who reach adult dimorphism values greater than the monkeys. We suggest that brain dimorphism is not likely to impose an additional energetic burden to the gestating or lactating mother. Finally, some of the problems with ascribing functional significance to brain size sexual dimorphism are discussed, and the energetic implications for brain size sexual dimorphism in infancy are assessed. [ABSTRACT FROM AUTHOR]

Published

2005

15. Fetal gender determination in early first trimester pregnancies of rhesus monkeys ( Macaca mulatta) by fluorescent PCR analysis of maternal serum.

Author

Jimenez, Daniel F. and Tarantal, Alice F.

Subjects

*SERUM, *RHESUS monkeys, *POLYMERASE chain reaction, *GENDER

Abstract

Jimenez DF, Tarantal AF. Fetal gender determination in early first trimester pregnancies of rhesus monkeys ( Macaca mulatta) by fluorescent PCR analysis of maternal serum. J Med Primatol 2003; 32:315–319. © Blackwell Munksgaard, 2003 Non-human primate fetal gender determination can be a powerful tool for research study design and colony management purposes. The recent discovery of the presence of fetal DNA in maternal serum has offered a new non-invasive approach for identification of fetal gender. We present a rapid and simple method for the sexing of developing rhesus monkeys in the first trimester by polymerase chain reaction (PCR) analysis of maternal serum. Serum samples were obtained from 72 gravid rhesus monkeys during 20–32 days of gestation (term 165 ± 10 days) . Fetal gender and the quantity of circulating fetal DNA were determined by real-time PCR analysis of the rhesus Y-chromosomal DNA sequences. The sensitivity for identifying a male fetus was 100% by 30 days gestation, and no false-positive results were observed. This study demonstrates that fetal gender can be reliably determined in the early first trimester from maternal serum samples, a non-invasive method for routine gender screening. [ABSTRACT FROM AUTHOR]

Published

2003

16. Tenofovir treatment at 30 mg/kg/day can inhibit cortical bone mineralization in growing rhesus monkeys (Macaca mulatta)

Author

Castillo, Alesha B., Tarantal, Alice F., Watnik, Mitchell R., and Bruce Martin, R.

Subjects

*NUCLEOSIDES, *IMMUNODEFICIENCY, *BIOMINERALIZATION

Abstract

The acyclic nucleoside phosphonate analog, 9-[2-(R)-(phosphonomethoxy)propyl]adenine (PMPA; Tenofovir; Gilead Sciences, Inc., Foster City, CA), has been shown to effectively inhibit simian immunodeficiency virus (SIV) replication in rhesus macaques by blocking reverse transcription. However, chronic long-term tenofovir treatment at 30 mg/kg/day, intended to reduce viral replication and illness, has been shown to result in bone deformities and spontaneous fractures in rhesus monkeys. Based on these findings, we studied the effects of tenofovir treatment and pathogenic SIV infection on cortical bone remodeling in rhesus monkeys. Tibiae from tenofovir-treated or untreated, SIV-infected or uninfected, rhesus macaques were evaluated for bone microdamage and remodeling. We found that tenofovir treatment had a significant effect on osteoid (unmineralized bone) seam width in tibial cross-sections. Regardless of SIV infection status, half of the tenofovir-treated animals had significantly increased osteoid seam widths in tibial cortical bone resulting in an osteomalacia-like condition. Pathogenic SIV infection significantly increased tibial resorption cavity density, and this increase was normalized by tenofovir treatment. These results suggest that tenofovir treatment at 30 mg/kg/day inhibits mineralization of newly formed bone. SIV infection results in increased tibial resorption cavity density, while tenofovir treatment tends to minimize this increase. Both defective mineralization of newly formed bone and increased resorption cavity density may result in greater bone fragility. [Copyright &y& Elsevier]

Published

2002

17. Experimental models of fetal obstructive nephropathy.

Author

Matsell, Douglas G. and Tarantal, Alice F.

Subjects

*KIDNEY diseases, *DYSPLASIA

Abstract

Urinary tract obstruction in the developing human fetus is an important cause of postnatal kidney failure and is the most common cause of end-stage renal disease and chronic renal failure in boys less than 4 years of age. Although the pathogenesis of renal dysplasia resulting from urinary tract obstruction is not well defined, it is clear that the earlier the obstruction occurs during in utero nephrogenesis the more severe the histopathological changes. Efforts to intervene in the human fetus have been hampered by an inaccuracy of diagnosis and by a lack of validation of in utero features predictive of poor outcome. A number of experimental models of obstructive renal dysplasia have been developed, which result in the consistent histopathological features of tubular cell apoptosis, mesenchymal expansion with mesenchymal myocyte transformation, and decreased glomerular endowment and glomerular injury. Defining the optimal timing of release of obstruction and restoring normal developmental gene and protein patterns should guide future intervention in these processes. Experimental animal models that closely simulate human development and disease will, thus, be essential for exploring these questions, and for assessing novel fetal therapies for future human application. [ABSTRACT FROM AUTHOR]

Published

2002

18. Fetal and Maternal Outcome After Administration of Tenofovir to Gravid Rhesus Monkeys (Macaca mullatta).

Author

Tarantal, Alice F., Castillo, Alesha, Ekert, Jason E., Bischofberger, Norbert, and Martin, R. Bruce

Subjects

*LABORATORY monkeys, *RHESUS monkeys, *THERAPEUTICS, *HIV infections

Abstract

Discusses fetal and maternal results of tenofovir administration to gravid rhesus monkeys in an effort to investigate treatment of HIV infection. Details of tenofovir preparation and treatment; Information on the bone-related toxicity of tenofovir; Fetal and maternal evaluations and sample collection.

Published

2002

19. Fetal rhesus monkey model of obstructive renal dysplasia.

Author

Tarantal, Alice F., Han, Victor K.M., Cochrum, Kent C., Mok, Amy, DaSilva, Michael, Matsell, Douglas G., Tarantal, A F, Han, V K, Cochrum, K C, Mok, A, daSilva, M, and Matsell, D G

Subjects

*ANIMAL models in research, *KIDNEY diseases

Abstract

Background: Disorders of kidney development represent a major cause of renal failure and end-stage renal disease in the pediatric population. To understand further the prenatal pathogenesis of obstructive renal dysplasia, a fetal monkey model was developed using ultrasound-guided techniques. Methods: Ureteropelvic obstruction (N = 13) was induced during the early or late second trimester by the injection of purified guluronic alginate spheres. All fetuses were monitored sonographically, and then fetal tissues were removed at varying time points during the second and third trimesters. Results: There was no evidence of oligohydramnios during the course of gestation, and the obstructed kidneys were typically progressively smaller than the contralateral (nonobstructed) kidneys when monitored sonographically over time. Obstructed kidneys displayed most features of renal dysplasia, including numerous cortical cysts of various sizes derived predominantly from collecting ducts and glomeruli. Mesenchymal changes included expansion of both the cortical and medullary interstitium, as well as mesenchymal-myocyte transformation, expressed as pericystic and peritubular fibromuscular collar formation. An important feature of this model was the disruption of normal glomerular development and architecture, associated with significant podocyte apoptosis, evident as early as the prevascularized S-shaped nephron. As in other models, collecting duct cell apoptosis was apparent, particularly in areas of cyst formation and cellular atrophy. Conclusions: These results demonstrate the importance of this nonhuman primate model for exploring the pathophysiology of congenital obstructive uropathy and highlight the potential role of podocyte injury in determining long-term renal function associated with this condition. [ABSTRACT FROM AUTHOR]

Published

2001

20. AAV5 Delivery of CRISPR/Cas9 Mediates Genome Editing in the Lungs of Young Rhesus Monkeys.

Author

Liang, Shun-Qing, Navia, Andrew W., Ramseier, Michelle, Zhou, Xuntao, Martinez, Michele, Lee, Charles, Zhou, Chen, Wu, Joae, Xie, Jun, Su, Qin, Wang, Dan, Flotte, Terence R., Anderson, Daniel G., Tarantal, Alice F., Shalek, Alex K., Gao, Guangping, and Xue, Wen

Subjects

*RHESUS monkeys, *GENOME editing, *ANGIOTENSIN converting enzyme, *RNA sequencing, *CRISPRS, *LUNGS

Abstract

Genome editing has the potential to treat genetic diseases in a variety of tissues, including the lung. We have previously developed and validated a dual adeno-associated virus (AAV) CRISPR platform that supports effective editing in the airways of mice. To validate this delivery vehicle in a large animal model, we have shown that intratracheal instillation of CRISPR/Cas9 in AAV5 can edit a housekeeping gene or a disease-related gene in the lungs of young rhesus monkeys. We observed up to 8% editing of angiotensin-converting enzyme 2 (ACE2) in lung lobes after single-dose administration. Single-nuclear RNA sequencing revealed that AAV5 transduces multiple cell types in the caudal lung lobes, including alveolar cells, macrophages, fibroblasts, endothelial cells, and B cells. These results demonstrate that AAV5 is efficient in the delivery of CRISPR/Cas9 in the lung lobes of young rhesus monkeys. [ABSTRACT FROM AUTHOR]

Published

2024

21. Administration of 9-[2-(R)-(phosphonomethoxy)propyl]adenine (PMPA) to Gravid and Infant Rhesus...

Author

Tarantal, Alice F. and Marthas, Marta L.

Subjects

*VIROLOGY, *PLACENTA, *PHARMACOKINETICS, *EXAMINATIONS

Abstract

Presents information on a study which determined the safety and efficacy of 9-[2-(R)-(phosphonomethoxy)propyl]adenine (PMPA) in virology. Exploration of placental transport of PMPA; Assessment of pharmacokinetic parameters in the fetus, infant and dam; Indications of the study.

Published

1999

22. Effects of viral virulence on intrauterine growth in SIV-infected fetal rhesus macaques...

Author

Tarantal, Alice F. and Marthas, Marta L.

Subjects

*SIMIAN viruses, *VIRUS diseases, *FETAL development, *PATHOLOGY

Abstract

Examines a simian immunodeficiency virus (SIV)-infected fetal monkey focusing on fetal growth and viral pathogenesis. Inoculation of fetuses in utero via ultrasound guidance; Peripheral blood hematologic and endocrine studies.

Published

1995

23. Infant Mortality: The Role of the Macaque as a Model for Human Disease.

Author

Hendricky, Andrew G. and Tarantal, Alice F.

Subjects

*INFANT mortality, *MACAQUES, *ANIMAL models in research, *HUMAN abnormalities, *CELL transplantation, *HEMOGLOBINOPATHY, *SUDDEN infant death syndrome

Abstract

Factors which have been identified as the leading causes of infant mortality include birth defects, hemoglobinopathies, prematurity, and Sudden Infant Death Syndrome (SIDS). In order to further our understanding of the specific causes of infant mortality and the mechanisms by which they occur, suitable animal models will be required. Studies with nonhuman primates (specifically the macaque) have addressed malformation/functional deficit syndromes such as those associated with Fetal Alcohol Syndrome (FAS), nutritional deficiencies, and retinoid teratogenicity. These studies have provided critical information for further basic and preventive research. In addition, efforts to evaluate the safety of diagnostic ultrasound continue to aid in identifying safe methods for exposure. From a prenatal perspective, cellular transplantation has been shown to be a feasible method for treating individuals with inherited defects in utero, thereby avoiding postnatal transplantation and the associated risks. Long-term complications for prematurity have also been pursued with growth factors (i.e., epidermal growth factor) noted to play an important role in both pre- and postnatal development of the gastrointestinal tract and lung. As one of the most distressing causes of death in infancy, SIDS will require a concentrated effort to understand the basic mechanism(s) responsible for the characteristic respiratory complications. The nonhuman primate will continue to provide critical information as the model of choice for the human in determining the causes, mechanisms, and treatments for these significant causes of infant death. [ABSTRACT FROM AUTHOR]

Published

1994

24. Hematologic Reference Values for the Fetal Long-Tailed Macaque (Macaca fascicularis).

Author

Tarantal, Alice F.

Subjects

*MACAQUES, *CORD blood, *CERCOPITHECIDAE, *BLOOD testing, *FETUS, *PRIMATES

Abstract

Complete blood counts (CBCs) were performed on 68 fetal macaque blood samples collected from 31 fetuses by repeat ultrasound-guided cardiocentesis (gestational day [GD] 80-150; term ∼ GD 165) with the goal of defining normative hematologic reference values during prenatal life. Lymphocytes were the primary white blood cells (WBCs) observed throughout gestation. Segmented neutrophils were the second highest percent of WBCs and were noted to rise significantly during GD 130-140. Overall, WBCs increased progressively throughout gestation with a transient decline at the beginning of the third trimester (∼ GD 110). A steady linear rise in red blood cells (RBCs), hemoglobin, and hematocrit was observed with a marginal decline close to term; mean corpuscular hemoglobin (MCH) and mean corpuscular volume (MCV) showed a consistent linear decline throughout gestation whereas mean corpuscular hemoglobin concentration (MCHC) remained relatively stable. Nucleated RBCs (NRBCs per 100 WBCs) were present on GD 80, showed a sharp decline mid-second trimester (∼ GD 90), and were significantly diminished by the beginning of the third trimester (∼ GD 110). No quantitative changes in platelets were noted throughout the study period. Evaluations of erythrocyte morphology indicated polychromasia and anisocytosis as typical characteristics throughout gestation with rare occurrence of hypochromasia and poikilocytosis. Howell-Jolly bodies were intermittently observed. These data reveal distinct similarities when compared to prenatal hematologic characteristics for human fetuses and provide baseline data which can be applied to experimental studies where prenatal hematopoietic/hematologic toxicity may be anticipated. [ABSTRACT FROM AUTHOR]

Published

1993

25. Mathematical Modeling of Rhesus Cytomegalovirus Transplacental Transmission in Seronegative Rhesus Macaques.

Author

Gong, Yishu, Moström, Matilda, Otero, Claire, Valencia, Sarah, Tarantal, Alice F., Kaur, Amitinder, Permar, Sallie R., and Chan, Cliburn

Subjects

*VERTICAL transmission (Communicable diseases), *FETAL diseases, *MACAQUES, *CONGENITAL disorders, *CYTOMEGALOVIRUS diseases, *CYTOMEGALOVIRUSES, *RHESUS monkeys

Abstract

Approximately 0.7% of infants are born with congenital cytomegalovirus (CMV), making it the most common congenital infection. About 1 in 5 congenitally infected babies will suffer long-term sequelae, including sensorineural deafness, intellectual disability, and epilepsy. CMV infection is highly species-dependent, and the rhesus CMV (RhCMV) infection of rhesus monkey fetuses is the only animal model that replicates essential features of congenital CMV (cCMV) infection in humans, including placental transmission, fetal disease, and fetal loss. Using experimental data from RhCMV seronegative rhesus macaques inoculated with RhCMV in the late first to early second trimesters of pregnancy, we built and calibrated a mathematical model for the placental transmission of CMV. The model was then used to study the effect of the timing of inoculation, maternal immune suppression, and hyper-immune globulin infusion on the risk of placental transmission in the context of primary and reactivated chronic maternal CMV infection. [ABSTRACT FROM AUTHOR]

Published

2023

26. 743. Lentiviral Vector Gene Transfer in Monkeys: In Vivo. Detection of Gene Expression Longitudinally Using MicroPET and Optical Imaging

Author

Tarantal, Alice F., Lee, Chang I., Jimenez, Daniel F., Gambhir, Sanjiv S., Kohn, Donald B., Rossi, John J., and Cherry, Simon R.

Subjects

*LENTIVIRUSES, *GENE expression

Abstract

An abstract of the article "Lentiviral Vector Gene Transfer in Monkeys: In Vivo Detection of Gene Expression Longitudinally Using MicroPET and Optical Imaging," by Alice F. Tarantal, Chang I. Lee, Daniel F. Jimenez, Sanjiv S. Gambhir, Donald B. Kohn, John J. Rossi and Simon R. Cherry is presented.

Published

2005

27. 462. Busulfan Dose Escalation to Increase Gene Marking of Hematopoietic Stem Cells by Lentiviral Vectors in Infant Rhesus Monkeys

Author

Kahl, Christoph A., Tarantal, Alice F., Lee, Chang I., Jimenez, Daniel F., Choi, Christopher, Pepper, Karen, Peterson, Denise, Fletcher, Misty D., Leapley, Alyssa C., and Kohn, Donald B.

Subjects

*HEMATOPOIETIC stem cells, *RHESUS monkeys

Abstract

An abstract of the article "Busulfan Dose Escalation to Increase Gene Marking of Hematopoietic Stem Cells by Lentiviral Vectors in Infant Rhesus Monkeys," by Christoph A. Kahl and colleagues is presented.

Published

2005

28. Natural Scaffolds for Renal Differentiation of Human Embryonic Stem Cells for Kidney Tissue Engineering.

Author

Batchelder, Cynthia A., Martinez, Michele L., and Tarantal, Alice F.

Subjects

*EMBRYONIC stem cells, *TISSUE engineering, *BIOENGINEERING, *TRANSPLANTATION of organs, tissues, etc., *TISSUE scaffolds, *EXTRACELLULAR matrix

Abstract

Despite the enthusiasm for bioengineering of functional renal tissues for transplantation, many obstacles remain before the potential of this technology can be realized in a clinical setting. Viable tissue engineering strategies for the kidney require identification of the necessary cell populations, efficient scaffolds, and the 3D culture conditions to develop and support the unique architecture and physiological function of this vital organ. Our studies have previously demonstrated that decellularized sections of rhesus monkey kidneys of all age groups provide a natural extracellular matrix (ECM) with sufficient structural properties with spatial and organizational influences on human embryonic stem cell (hESC) migration and differentiation. To further explore the use of decellularized natural kidney scaffolds for renal tissue engineering, pluripotent hESC were seeded in whole- or on sections of kidney ECM and cell migration and phenotype compared with the established differentiation assays for hESC. Results of qPCR and immunohistochemical analyses demonstrated upregulation of renal lineage markers when hESC were cultured in decellularized scaffolds without cytokine or growth factor stimulation, suggesting a role for the ECM in directing renal lineage differentiation. hESC were also differentiated with growth factors and compared when seeded on renal ECM or a new biologically inert polysaccharide scaffold for further maturation. Renal lineage markers were progressively upregulated over time on both scaffolds and hESC were shown to express signature genes of renal progenitor, proximal tubule, endothelial, and collecting duct populations. These findings suggest that natural scaffolds enhance expression of renal lineage markers particularly when compared to embryoid body culture. The results of these studies show the capabilities of a novel polysaccharide scaffold to aid in defining a protocol for renal progenitor differentiation from hESC, and advance the promise of tissue engineering as a source of functional kidney tissue. [ABSTRACT FROM AUTHOR]

Published

2015

29. Imaging the fetal nonhuman primate brain with SV2A positron emission tomography (PET).

Author

Rossano, Samantha, Toyonaga, Takuya, Berg, Eric, Lorence, Isabella, Fowles, Krista, Nabulsi, Nabeel, Ropchan, Jim, Li, Songye, Ye, Yunpeng, Felchner, Zachary, Kukis, David, Huang, Yiyun, Benveniste, Helene, Tarantal, Alice F., Groman, Stephanie, and Carson, Richard E.

Subjects

*POSITRON emission tomography, *FETAL imaging, *SYNAPSES, *FETAL brain, *SYNAPTIC vesicles, *FETAL development

Abstract

Purpose: Exploring synaptic density changes during brain growth is crucial to understanding brain development. Previous studies in nonhuman primates report a rapid increase in synapse number between the late gestational period and the early neonatal period, such that synaptic density approaches adult levels by birth. Prenatal synaptic development may have an enduring impact on postnatal brain development, but precisely how synaptic density changes in utero are unknown because current methods to quantify synaptic density are invasive and require post-mortem brain tissue. Methods: We used synaptic vesicle glycoprotein 2A (SV2A) positron emission tomography (PET) radioligands [11C]UCB-J and [18F]Syn-VesT-1 to conduct the first assessment of synaptic density in the developing fetal brain in gravid rhesus monkeys. Eight pregnant monkeys were scanned twice during the third trimester at two imaging sites. Fetal post-mortem samples were collected near term in a subset of subjects to quantify SV2A density by Western blot. Results: Image-derived fetal brain SV2A measures increased during the third trimester. SV2A concentrations were greater in subcortical regions than in cortical regions at both gestational ages. Near term, SV2A density was higher in primary motor and visual areas than respective associative regions. Post-mortem quantification of SV2A density was significantly correlated with regional SV2A PET measures. Conclusion: While further study is needed to determine the exact relationship of SV2A and synaptic density, the imaging paradigm developed in the current study allows for the effective in vivo study of SV2A development in the fetal brain. [ABSTRACT FROM AUTHOR]

Published

2022

30. Analysis of maternal microchimerism in rhesus monkeys (Macaca mulatta) using real-time quantitative PCR amplification of MHC polymorphisms.

Author

Bakkour, Sonia, Baker, Chris A. R., Tarantal, Alice F., Li Wen, Busch, Michael P., Tzong-Hae Lee, and Mccune, Joseph M.

Subjects

*CHIMERISM, *RHESUS monkeys, *ANIMAL young, *POLYMERASE chain reaction, *CELL analysis

Abstract

Although pregnancy-associated microchimerism is known to exist in humans, its clinical significance remains unclear. Fetal microchimerism has been documented in rhesus monkeys, but the trafficking and persistence of maternal cells in the monkey fetus and infant have not been fully explored. To investigate the frequency of maternal microchimerism in the rhesus monkey (Macaca mulatta), a real-time polymerase chain reaction (PCR) strategy was developed and validated to target polymorphic major histocompatibility complex (MHC) gene sequences. Informative PCR assays were identified for 19 of 25 dams and their respective offspring. analyses were performed on tissues (thymus, liver, spleen, lymph nodes, and bone marrow) and peripheral blood mononuclear cells (PBMCs) collected prenatally and postnatally in a subset of animals. Seven of 19 monkeys had detectable maternal microchimerism in at least one compartment (range: 0.001-1.9% chimeric cells). In tissues, maternal microchimerism was found in 2 of 7 fetuses and 3 of 12 juveniles (1-1.5 years of age), and most of the animals that were positive had microchimeric cells in more than one tissue. Maternal microchimerism was detected in PBMCs from all (4 of 4) fetuses. These observations suggest that maternal microchimerism occurs in the rhesus monkey fetus and can be detected in tissues in a subset of offspring after birth. [ABSTRACT FROM AUTHOR]

Published

2014

31. Visual recognition memory and auditory brainstem response in infant rhesus monkeys exposed perinatally to environmental tobacco smoke

Author

Golub, Mari S., Slotkin, Theodore A., Tarantal, Alice F., and Pinkerton, Kent E.

Subjects

*VISUAL perception, *RHESUS monkeys, *PHYSIOLOGICAL effects of smoke, *COGNITIVE development

Abstract

Abstract: The impact of perinatal exposure to environmental tobacco smoke (ETS) on cognitive development is controversial. We exposed rhesus monkeys to ETS or filtered air (5 animals per group) beginning in utero on day 50 of pregnancy and continuing throughout postnatal testing. In infancy, we evaluated both groups for visual recognition memory and auditory function (auditory brainstem response). The ETS group showed significantly less novelty preference in the visual recognition task whereas no effects on auditory function were detected. These preliminary results support the view that perinatal ETS exposure has adverse effects on cognitive function and indicate further that rhesus monkeys may provide a valuable nonhuman primate model for investigating this link. [Copyright &y& Elsevier]

Published

2007

32. Altered primate glomerular development due to in utero urinary tract obstruction.

Author

Matsell, Douglas G, Mok, Amy, and Tarantal, Alice F

Subjects

*URINATION disorders, *PEDIATRIC nephrology

Abstract

Background. In utero urinary tract obstruction is an important cause of newborn and childhood renal failure. Ureteric obstruction during active nephrogenesis results in cystic renal dysplasia; the earlier and longer the obstruction the more severe the histopathological changes of dysplasia. We have reported on a non-human primate model of non-surgical in utero fetal ureteric obstruction that accurately reflects the human equivalent of obstructive renal dysplasia. A striking feature of this model is the effect of obstruction on normal glomerular development and podocyte survival. Methods. To study the effect of urinary obstruction on glomerular development, kidneys were studied from fetuses undergoing unilateral ureteric obstruction by ultrasound guided injection of alginate beads as early as 75 days gestation (term gestation = 165 ± 10 days). These kidneys displayed all the features of human obstructive cystic dysplasia, had reduced weights, and significant deficiencies in terminal ureteric duct branching. Results. A combination of histochemistry, histomorphometry, and immunocytochemistry was used to demonstrate deficient cortical ureteric duct development and branching, reduced glomerular number, and altered glomerular basement membrane formation with in utero urinary tract obstruction. Conclusions. These data suggest that urinary tract obstruction during active nephrogenesis results in a defect in ureteric duct branching morphogenesis, and altered vascularization of the glomerulus with consequent podocyte dropout and decreased glomerular number. These abnormalities reflect human renal dysplasia, which is associated with compromised postnatal renal function and, thus, should be predictive of postnatal outcome. [ABSTRACT FROM AUTHOR]

Published

2002

33. Greater Number of Microglia in Telencephalic Proliferative Zones of Human and Nonhuman Primate Compared with Other Vertebrate Species.

Author

Penna, Elisa, Cunningham, Christopher L, Saylor, Stephanie, Kreutz, Anna, Tarantal, Alice F, Martínez-Cerdeño, Verónica, and Noctor, Stephen C

Subjects

*FRACTALKINE, *RATS, *MICROGLIA, *PRIMATES, *VERTEBRATES, *SPECIES

Abstract

Microglial cells, the innate immune cells of the brain, are derived from yolk sac precursor cells, begin to colonize the telencephalon at the onset of cortical neurogenesis, and occupy specific layers including the telencephalic proliferative zones. Microglia are an intrinsic component of cortical germinal zones, establish extensive contacts with neural precursor cells (NPCs) and developing cortical vessels, and regulate the size of the NPC pool through mechanisms that include phagocytosis. Microglia exhibit notable differences in number and distribution in the prenatal neocortex between rat and old world nonhuman primate telencephalon, suggesting that microglia possess distinct properties across vertebrate species. To begin addressing this subject, we quantified the number of microglia and NPCs in proliferative zones of the fetal human, rhesus monkey, ferret, and rat, and the prehatch chick and turtle telencephalon. We show that the ratio of NPCs to microglia varies significantly across species. Few microglia populate the prehatch chick telencephalon, but the number of microglia approaches that of NPCs in fetal human and nonhuman primate telencephalon. These data demonstrate that microglia are in a position to perform important functions in a number of vertebrate species but more heavily colonize proliferative zones of fetal human and rhesus monkey telencephalon. [ABSTRACT FROM AUTHOR]

Published

2021

34. Transcriptome analysis of non human primate-induced pluripotent stem cell-derived cardiomyocytes in 2D monolayer culture vs. 3D engineered heart tissue.

Author

Yang, Huaxiao, Shao, Ningyi, Holmström, Alexandra, Zhao, Xin, Chour, Tony, Chen, Haodong, Itzhaki, Ilanit, Wu, Haodi, Ameen, Mohamed, Cunningham, Nathan J, Tu, Chengyi, Zhao, Ming-Tao, Tarantal, Alice F, Abilez, Oscar J, and Wu, Joseph C

Subjects

*STEM cell treatment, *MONOMOLECULAR films, *RHESUS monkeys, *HEART, *TISSUES

Abstract

Aims Stem cell therapy has shown promise for treating myocardial infarction via re-muscularization and paracrine signalling in both small and large animals. Non-human primates (NHPs), such as rhesus macaques (Macaca mulatta), are primarily utilized in preclinical trials due to their similarity to humans, both genetically and physiologically. Currently, induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) are delivered into the infarcted myocardium by either direct cell injection or an engineered tissue patch. Although both approaches have advantages in terms of sample preparation, cell–host interaction, and engraftment, how the iPSC-CMs respond to ischaemic conditions in the infarcted heart under these two different delivery approaches remains unclear. Here, we aim to gain a better understanding of the effects of hypoxia on iPSC-CMs at the transcriptome level. Methods and results NHP iPSC-CMs in both monolayer culture (2D) and engineered heart tissue (EHT) (3D) format were exposed to hypoxic conditions to serve as surrogates of direct cell injection and tissue implantation in vivo , respectively. Outcomes were compared at the transcriptome level. We found the 3D EHT model was more sensitive to ischaemic conditions and similar to the native in vivo myocardium in terms of cell–extracellular matrix/cell–cell interactions, energy metabolism, and paracrine signalling. Conclusion By exposing NHP iPSC-CMs to different culture conditions, transcriptome profiling improves our understanding of the mechanism of ischaemic injury. [ABSTRACT FROM AUTHOR]

Published

2021

35. A primary Chlamydia trachomatis genital infection of rhesus macaques identifies new immunodominant B-cell antigens.

Author

Randall, Arlo, Teng, Andy, Liang, Xiaowu, Pal, Sukumar, Tarantal, Alice F., Fike, Joseph, Barry, Peter A., and de la Maza, Luis M.

Subjects

*MACAQUES, *CHLAMYDIA trachomatis, *RHESUS monkeys, *ANTIGENS, *B cells, *HUMORAL immunity, *INFECTION

Abstract

To identify immunodominant antigens that elicit a humoral immune response following a primary and a secondary genital infection, rhesus monkeys were inoculated cervically with Chlamydia trachomatis serovar D. Serum samples were collected and probed with a protein microarray expressing 864/894 (96.4%) of the open reading frames of the C. trachomatis serovar D genome. The antibody response to the primary infection was analyzed in 72 serum samples from 12 inoculated monkeys. The following criteria were utilized to identify immunodominant antigens: proteins found to be recognized by at least 75% (9/12) of the infected monkeys with at least 15% elevations in signal intensity from week 0 to week 8 post infection. All infected monkeys developed Chlamydia specific serum antibodies. Eight proteins satisfied the selection criteria for immunodominant antigens: CT242 (OmpH-like protein), CT541 (mip), CT681 (ompA), CT381 (artJ), CT443 (omcB), CT119 (incA), CT486 (fliY), and CT110 (groEL). Of these, three antigens, CT119, CT486 and CT381, were not previously identified as immunodominant antigens using non-human primate sera. Following the secondary infection, the antibody responses to the eight immunodominant antigens were analyzed and found to be quite different in intensity and duration to the primary infection. In conclusion, these eight immunodominant antigens can now be tested for their ability to identify individuals with a primary C. trachomatis genital infection and to design vaccine strategies to protect against a primary infection with this pathogen. [ABSTRACT FROM AUTHOR]

Published

2021

36. Safe and Sustained Expression of Human Iduronidase After Intrathecal Administration of Adeno-Associated Virus Serotype 9 in Infant Rhesus Monkeys.

Author

Hordeaux, Juliette, Hinderer, Christian, Buza, Elizabeth L., Louboutin, Jean-Pierre, Jahan, Tahsin, Bell, Peter, Chichester, Jessica A., Tarantal, Alice F., and Wilson, James M.

Subjects

*TRANSGENE expression, *RHESUS monkeys, *ADENO-associated virus, *DORSAL root ganglia, *PURKINJE cells, *MOTOR neurons, *PYRAMIDAL neurons, *CEREBROSPINAL fluid

Abstract

Many neuropathic diseases cause early, irreversible neurologic deterioration, which warrants therapeutic intervention during the first months of life. In the case of mucopolysaccharidosis type I, a recessive lysosomal storage disorder that results from a deficiency of the lysosomal enzyme α-l-iduronidase (IDUA), one of the most promising treatment approaches is to restore enzyme expression through gene therapy. Specifically, administering pantropic adeno-associated virus (AAV) encoding IDUA into the cerebrospinal fluid (CSF) via suboccipital administration has demonstrated remarkable efficacy in large animals. Preclinical safety studies conducted in adult nonhuman primates supported a positive risk–benefit profile of the procedure while highlighting potential subclinical toxicity to primary sensory neurons located in the dorsal root ganglia (DRG). This study investigated the long-term performance of intrathecal cervical AAV serotype 9 gene transfer of human IDUA administered to 1-month-old rhesus monkeys (N = 4) with half of the animals tolerized to the human transgene at birth via systemic administration of an AAV serotype 8 vector expressing human IDUA from the liver. Sustained expression of the transgene for almost 4 years is reported in all animals. Transduced cells were primarily pyramidal neurons in the cortex and hippocampus, Purkinje cells in the cerebellum, lower motor neurons, and DRG neurons. Both tolerized and non-tolerized animals were robust and maintained transgene expression as measured by immunohistochemical analysis of brain tissue. However, the presence of antibodies in the non-tolerized animals led to a loss of measurable levels of secreted enzyme in the CSF. These results support the safety and efficiency of treating neonatal rhesus monkeys with AAV serotype 9 gene therapy delivered into the CSF. [ABSTRACT FROM AUTHOR]

Published

2019

37. Periventricular microglial cells interact with dividing precursor cells in the nonhuman primate and rodent prenatal cerebral cortex.

Author

Noctor, Stephen C., Penna, Elisa, Shepherd, Hunter, Chelson, Christian, Barger, Nicole, Martínez‐Cerdeño, Verónica, and Tarantal, Alice F.

Abstract

Cortical proliferative zones have been studied for over 100 years, yet recent data have revealed that microglial cells constitute a sizeable proportion of ventricular zone cells during late stages of cortical neurogenesis. Microglia begin colonizing the forebrain after neural tube closure and during later stages of neurogenesis populate regions of the developing cortex that include the proliferative zones. We previously showed that microglia regulate the production of cortical cells by phagocytosing neural precursor cells (NPCs), but how microglia interact with NPCs remains poorly understood. Here we report on a distinct subset of microglial cells, which we term periventricular microglia, that are located near the lateral ventricle in the prenatal neocortex. Periventricular microglia exhibit a set of similar characteristics in embryonic rat and fetal rhesus monkey cortex. In both species, these cells occupy ~60 μm of the ventricular zone in the tangential axis and make contact with the soma and processes of NPCs dividing at the ventricle for over 50 μm along the radial axis. Periventricular microglia exhibit notable differences across species, including distinct morphological features such as terminal bouton‐like structures that contact mitotic NPCs in the fetal rhesus monkey but not in rat. These morphological distinctions suggest differential functions of periventricular microglia in rat and rhesus monkey, yet are consistent with the concept that microglia regulate NPC function in the developing cerebral cortex of mammalian species. [ABSTRACT FROM AUTHOR]

Published

2019

38. Safety profile after prolonged C3 inhibition.

Author

Reis, Edimara S., Berger, Nadja, Wang, Xin, Koutsogiannaki, Sophia, Doot, Robert K., Gumas, Justin T., Foukas, Periklis G., Resuello, Ranillo R.G., Tuplano, Joel V., Kukis, David, Tarantal, Alice F., Young, Anthony J., Kajikawa, Tetsuhiro, Soulika, Athena M., Mastellos, Dimitrios C., Yancopoulou, Despina, Biglarnia, Ali-Reza, Huber-Lang, Markus, Hajishengallis, George, and Nilsson, Bo

Subjects

*IMMUNE response, *PHAGOCYTOSIS, *HEMATOLOGY, *RHESUS monkeys, *IMMUNE system

Abstract

Abstract The central component of the complement cascade, C3, is involved in various biological functions, including opsonization of foreign bodies, clearance of waste material, activation of immune cells, and triggering of pathways controlling development. Given its broad role in immune responses, particularly in phagocytosis and the clearance of microbes, a deficiency in complement C3 in humans is often associated with multiple bacterial infections. Interestingly, an increased susceptibility to infections appears to occur mainly in the first two years of life and then wanes throughout adulthood. In view of the well-established connection between C3 deficiency and infections, therapeutic inhibition of complement at the level of C3 is often considered with caution or disregarded. We therefore set out to investigate the immune and biochemical profile of non-human primates under prolonged treatment with the C3 inhibitor compstatin (Cp40 analog). Cynomolgus monkeys were dosed subcutaneously with Cp40, resulting in systemic inhibition of C3, for 1 week, 2 weeks, or 3 months. Plasma concentrations of both C3 and Cp40 were measured periodically and complete saturation of plasma C3 was confirmed. No differences in hematological, biochemical, or immunological parameters were identified in the blood or tissues of animals treated with Cp40 when compared to those injected with vehicle alone. Further, skin wounds showed no signs of infection in those treated with Cp40. In fact, Cp40 treatment was associated with a trend toward accelerated wound healing when compared with the control group. In addition, a biodistribution study in a rhesus monkey indicated that the distribution of Cp40 in the body is associated with the presence of C3, concentrating in organs that accumulate blood and produce C3. Overall, our data suggest that systemic C3 inhibition in healthy adult non-human primates is not associated with a weakened immune system or susceptibility to infections. [ABSTRACT FROM AUTHOR]

Published

2018

39. Maternal and Fetal Pharmacokinetics of Oral Radiolabeled and Authentic Bisphenol A in the Rhesus Monkey.

Author

VandeVoort, Catherine A., Gerona, Roy R., vom Saal, Frederick S., Tarantal, Alice F., Hunt, Patricia A., Hillenweck, Anne, and Zalko, Daniel

Subjects

*PHARMACOKINETICS, *RADIOLABELED blood cells, *BISPHENOL A, *METABOLITES, *SERUM

Abstract

The present study was conducted in pregnant rhesus monkeys to determine the rapidity and extent to which BPA reaches the fetal compartment following oral ingestion, and the 24-hr fate of BPA. To assess metabolism changes during the course of pregnancy, we compared BPA biotransformation during the second and third trimesters in the same animals, measuring the levels of sulfated, gluronidated, and free BPA in maternal serum, amniotic fluid, and fetal serum. All animals showed measurable unconjugated and conjugated BPA in the fetal compartment and slow clearance compared to maternal serum. There were higher levels of BPA-G in amniotic fluid at 150 days gestation compared to 100 days gestation, as well as higher levels of BPA-G than BPA-S. We also monitored 3H-BPA (and metabolites) in key tissues and excreta from a mother and fetus and from a non-pregnant female. The elimination of radioactivity was rapid, but residues were still detectable 24 hr after dosing in all tissues analyzed. These data suggest that, in primates, rapid maternal processing of BPA does not alleviate the risk of exposure to the developing fetus. This study elevates concerns about levels of current BPA human exposure from potentially a large number of unknown sources and the risks posed to developing fetuses. [ABSTRACT FROM AUTHOR]

Published

2016

40. Three Dimensional Culture of Human Renal Cell Carcinoma Organoids.

Author

Batchelder, Cynthia A., Martinez, Michele L., Duru, Nadire, Meyers, Frederick J., and Tarantal, Alice F.

Subjects

*RENAL cell carcinoma, *CELL culture, *THREE-dimensional imaging, *POLYMERASE chain reaction, *IMMUNOHISTOCHEMISTRY

Abstract

Renal cell carcinomas arise from the nephron but are heterogeneous in disease biology, clinical behavior, prognosis, and response to systemic therapy. Development of patient-specific in vitro models that efficiently and faithfully reproduce the in vivo phenotype may provide a means to develop personalized therapies for this diverse carcinoma. Studies to maintain and model tumor phenotypes in vitro were conducted with emerging three-dimensional culture techniques and natural scaffolding materials. Human renal cell carcinomas were individually characterized by histology, immunohistochemistry, and quantitative PCR to establish the characteristics of each tumor. Isolated cells were cultured on renal extracellular matrix and compared to a novel polysaccharide scaffold to assess cell-scaffold interactions, development of organoids, and maintenance of gene expression signatures over time in culture. Renal cell carcinomas cultured on renal extracellular matrix repopulated tubules or vessel lumens in renal pyramids and medullary rays, but cells were not observed in glomeruli or outer cortical regions of the scaffold. In the polysaccharide scaffold, renal cell carcinomas formed aggregates that were loosely attached to the scaffold or free-floating within the matrix. Molecular analysis of cell-scaffold constructs including immunohistochemistry and quantitative PCR demonstrated that individual tumor phenotypes could be sustained for up to 21 days in culture on both scaffolds, and in comparison to outcomes in two-dimensional monolayer cultures. The use of three-dimensional scaffolds to engineer a personalized in vitro renal cell carcinoma model provides opportunities to advance understanding of this disease. [ABSTRACT FROM AUTHOR]

Published

2015

41. Neonatal Systemic AAV Induces Tolerance to CNS Gene Therapy in MPS I Dogs and Nonhuman Primates.

Author

Hinderer, Christian, Bell, Peter, Louboutin, Jean-Pierre, Zhu, Yanqing, Yu, Hongwei, Lin, Gloria, Choa, Ruth, Gurda, Brittney L, Bagel, Jessica, O'Donnell, Patricia, Sikora, Tracey, Ruane, Therese, Wang, Ping, Tarantal, Alice F, Casal, Margret L, Haskins, Mark E, and Wilson, James M

Subjects

*ADENO-associated virus, *PARVOVIRUSES, *CENTRAL nervous system diseases, *MUCOPOLYSACCHARIDOSIS treatment, *CARBOHYDRATE metabolism disorders, *GENE therapy, *THERAPEUTICS

Abstract

The potential host immune response to a nonself protein poses a fundamental challenge for gene therapies targeting recessive diseases. We demonstrate in both dogs and nonhuman primates that liver-directed gene transfer using an adeno-associated virus (AAV) vector in neonates induces a persistent state of immunological tolerance to the transgene product, substantially improving the efficacy of subsequent vector administration targeting the central nervous system (CNS). We applied this approach to a canine model of mucopolysaccharidosis type I (MPS I), a progressive neuropathic lysosomal storage disease caused by deficient activity of the enzyme α-l-iduronidase (IDUA). MPS I dogs treated systemically in the first week of life with a vector expressing canine IDUA did not develop antibodies against the enzyme and exhibited robust expression in the CNS upon intrathecal AAV delivery at 1 month of age, resulting in complete correction of brain storage lesions. Newborn rhesus monkeys treated systemically with AAV vector expressing human IDUA developed tolerance to the transgene, resulting in high cerebrospinal fluid (CSF) IDUA expression and no antibody induction after subsequent CNS gene therapy. These findings suggest that inducing tolerance to the transgene product during a critical period in immunological development can improve the efficacy and safety of gene therapy. [ABSTRACT FROM AUTHOR]

Published

2015

42. Rhesus monkey ( Macaca mulatta) lipoprotein(a) and apolipoprotein(a): high frequency of small size apolipoprotein(a) isoforms.

Author

Enkhmaa, Byambaa, Abbuthalha, Adnan, Anuurad, Erdembileg, Zhang, Wei, Tarantal, Alice F., and Berglund, Lars

Subjects

*MONKEYS, *MACAQUES, *RHESUS monkeys, *APOLIPOPROTEIN A, *LIPOPROTEIN A

Abstract

Background Levels of lipoprotein(a), Lp(a), a genetically regulated independent cardiovascular risk factor present in humans and Old World monkeys, are impacted by the apolipoprotein(a), apo(a), gene. Allele-specific apo(a) levels, taking both the apo(a) genotypic and phenotypic characteristics into account, are useful markers to determine atherosclerotic cardiovascular risk. Methods We determined (i) the genetic variability of apo(a), (ii) Lp(a) levels, and (iii) allele-specific apo(a) levels in rhesus monkeys (n = 95). Results Lp(a) levels differed substantially between animals (range: 4-247 nmol/l) with a skewed distribution toward lower levels. Lp(a) and allele-specific apo(a) levels were inversely related to the number of apo(a) Kringle 4 (K4) repeats. The median apo(a) size was 23 K4 repeats, and the prevalence of a small size apo(a) (≤22 K4) was 43%. Conclusions Distribution of Lp(a) and allele-specific apo(a) levels in rhesus monkeys reflected the corresponding human patterns, but with a high prevalence of smaller apo(a) sizes. [ABSTRACT FROM AUTHOR]

Published

2015

43. Abnormal Infant Islet Morphology Precedes Insulin Resistance in PCOS-Like Monkeys.

Author

Nicol, Lindsey E., O’Brien, Timothy D., Dumesic, Daniel A., Grogan, Tristan, Tarantal, Alice F., and Abbott, David H.

Subjects

*INSULIN resistance, *POLYCYSTIC ovary syndrome, *TYPE 2 diabetes, *ANDROGENS, *LABORATORY monkeys, *HYPERINSULINISM, *METABOLIC syndrome

Abstract

Polycystic ovary syndrome (PCOS) is prevalent in reproductive-aged women and confounded by metabolic morbidities, including insulin resistance and type 2 diabetes. Although the etiology of PCOS is undefined, contribution of prenatal androgen (PA) exposure has been proposed in a rhesus monkey model as premenopausal PA female adults have PCOS-like phenotypes in addition to insulin resistance and decreased glucose tolerance. PA female infants exhibit relative hyperinsulinemia, suggesting prenatal sequelae of androgen excess on glucose metabolism and an antecedent to future metabolic disease. We assessed consequences of PA exposure on pancreatic islet morphology to identify evidence of programming on islet development. Islet counts and size were quantified and correlated with data from intravenous glucose tolerance tests (ivGTT) obtained from dams and their offspring. Average islet size was decreased in PA female infants along with corresponding increases in islet number, while islet fractional area was preserved. Infants also demonstrated an increase in both the proliferation marker Ki67 within islets and the beta to alpha cell ratio suggestive of enhanced beta cell expansion. PA adult females have reduced proportion of small islets without changes in proliferative or apoptotic markers, or in beta to alpha cell ratios. Together, these data suggest in utero androgen excess combined with mild maternal glucose intolerance alter infant and adult islet morphology, implicating deviant islet development. Marked infant, but subtle adult, morphological differences provide evidence of islet post-natal plasticity in adapting to changing physiologic demands: from insulin sensitivity and relative hypersecretion to insulin resistance and diminished insulin response to glucose in the mature PCOS-like phenotype. [ABSTRACT FROM AUTHOR]

Published

2014

44. Optimizing the transduction efficiency of capsid-modified AAV6 serotype vectors in primary human hematopoietic stem cells in vitro and in a xenograft mouse model in vivo.

Author

LIUJIANG SONG, KAUSS, M. ARIEL, KOPIN, ETANA, CHANDRA, MANASA, UL-HASAN, TAIHRA, MILLER, ERIN, JAYANDHARAN, GIRIDHARA R., RIVERS, ANGELA E., ASLANIDI, GEORGE V., CHEN LING, BAOZHENG LI, WENQIN MA, XIAOMIAO LI, ANDINO, LOURDES M., LI ZHONG, TARANTAL, ALICE F., YODER, MERVIN C., WONG JR., KAMEHAMEHA K., MENGQUN TAN, and CHATTERJEE, SASWATI

Subjects

*CAPSIDS, *NUCLEOCAPSIDS, *XENOGRAFTS, *LABORATORY mice, *HEMATOPOIETIC stem cells, *TRANSGENE expression, *GENE therapy

Abstract

Background aims. Although recombinant adeno-associated virus serotype 2 (AAV2) vectors have gained attention because of their safety and efficacy in numerous phase I/II clinical trials, their transduction efficiency in hematopoietic stem cells (HSCs) has been reported to be low. Only a few additional AAV serotype vectors have been evaluated, and comparative analyses of their transduction efficiency in HSCs from different species have not been performed. Methods. We evaluated the transduction efficiency of all available AAV serotype vectors (AAV1 through AAV10) in primary mouse, cynomolgus monkey and human HSCs. The transduction efficiency of the optimized AAV vectors was also evaluated in human HSCs in a murine xenograft model in vivo. Results. We observed that although there are only six amino acid differences between AAV1 and AAV6, AAV1, but not AAV6, transduced mouse HSCs well, whereas AAV6, but not AAV1, transduced human HSCs well. None of the 10 serotypes transduced cynomolgus monkey HSCs in vitro. We also evaluated the transduction efficiency of AAV6 vectors containing mutations in surface-exposed tyrosine residues. We observed that tyrosine (Y) to phenylalanine (F) point mutations in residues 445, 705 and 731 led to a significant increase in transgene expression in human HSCs in vitro and in a mouse xenograft model in vivo. Conclusions. These studies suggest that the tyrosine-mutant AAV6 serotype vectors are the most promising vectors for transducing human HSCs and that it is possible to increase further the transduction efficiency of these vectors for their potential use in HSC-based gene therapy in humans. [ABSTRACT FROM AUTHOR]

Published

2013

45. Intra-Amniotic IL-1β Induces Fetal Inflammation in Rhesus Monkeys and Alters the Regulatory T Cell/IL-17 Balance.

Author

Kallapur, Suhas G., Presicce, Pietro, Senthamaraikannan, Paranthaman, Alvarez, Manuel, Tarantal, Alice F., Miller, Lisa M., Jobe, Alan H., and Chougnet, Claire A.

Subjects

*INTERLEUKIN-1, *ANIMAL models of inflammation, *T cells, *FETAL diseases, *NEWBORN infant immunology, *NUCLEIC acid isolation methods, *IMMUNOHISTOCHEMISTRY, *CELL culture, *PHYSIOLOGY

Abstract

Very low birth weight preterm newborns are susceptible to the development of debilitating inflammatory diseases, many of which are associated with chorioamnionitis. To define the effects of chorioamnionitis on the fetal immune system, IL-1β was administered intra-amniotically at ~80% gestation in rhesus monkeys. IL-1β caused histological chorioamnionitis, as well as lung inflammation (infiltration of neutrophils or monocytes in the fetal airways). There were large increases in multiple proinflammatory cytokine mRNAs in the lungs at 24 h postadministration, which remained elevated relative to controls at 72 h. Intra-amniotic IL-1β also induced the sustained expression of the surfactant proteins in the lungs. Importantly, IL-1β significantly altered the balance between inflammatory and regulatory T cells. Twenty-four hours after IL-1β injection, the frequency of CD3+CD4+FOXP3+ T cells was decreased in lymphoid organs. In contrast, IL-17A–producing cells (CD3+CD4+, CD3+CD4−, and CD3−CD4− subsets) were increased in lymphoid organs. The frequency of IFN-γ–expressing cells did not change. In this model of a single exposure to an inflammatory trigger, CD3+CD4+FOXP3+ cells rebounded quickly, and their frequency was increased at 72 h compared with controls. IL-17 expression was also transient. Interestingly, the T cell profile alteration was confined to the lymphoid organs and not to circulating fetal T cells. Together, these results suggest that the chorioamnionitis-induced IL-1/IL-17 axis is involved in the severe inflammation that can develop in preterm newborns. Boosting regulatory T cells and/or controlling IL-17 may provide a means to ameliorate these abnormalities. [ABSTRACT FROM AUTHOR]

Published

2013

46. Tissue Specificity of Decellularized Rhesus Monkey Kidney and Lung Scaffolds

Author

Nakayama, Karina H., Lee, C. Chang I., Batchelder, Cynthia A., and Tarantal, Alice F.

Subjects

*TISSUE-specific antigens, *RHESUS monkeys, *TISSUE scaffolds, *KIDNEY physiology, *LUNG physiology, *TISSUE engineering, *EMBRYONIC stem cells

Abstract

Initial steps in establishing an optimal strategy for functional bioengineered tissues is generation of three-dimensional constructs containing cells with the appropriate organization and phenotype. To effectively utilize rhesus monkey decellularized kidney scaffolds, these studies evaluated two key parameters: (1) residual scaffold components after decellularization including proteomics analysis, and (2) the use of undifferentiated human embryonic stem cells (hESCs) for recellularization in order to explore cellular differentiation in a tissue-specific manner. Sections of kidney and lung were selected for a comparative evaluation because of their similar pattern of organogenesis. Proteomics analysis revealed the presence of growth factors and antimicrobial proteins as well as stress proteins and complement components. Immunohistochemistry of recellularized kidney scaffolds showed the generation of Cytokeratin+ epithelial tubule phenotypes throughout the scaffold that demonstrated a statistically significant increase in expression of kidney-associated genes compared to baseline hESC gene expression. Recellularization of lung scaffolds showed that cells lined the alveolar spaces and demonstrated statistically significant upregulation of key lung-associated genes. However, overall expression of kidney and lung-associated markers was not statistically different when the kidney and lung recellularized scaffolds were compared. These results suggest that decellularized scaffolds have an intrinsic spatial ability to influence hESC differentiation by physically shaping cells into tissue-appropriate structures and phenotypes, and that additional approaches may be needed to ensure consistent recellularization throughout the matrix. [ABSTRACT FROM AUTHOR]

Published

2013

47. AAV-mediated gene transfer in the perinatal period results in expression of FYII at levels that protect against fatal spontaneous hemorrhage.

Author

Binny, Christopher, McIntosh, Jenny, Peruta, Marco Della, Kymalainen, Hanna, Tuddenham, Edward G. D., Buckley, Suzanne M. K., Waddington, Simon N., McVey, John H., Spence, Yunyu, Morton, Christopher L., Thrasher, Adrian J., Gray, John T., Castellino, Francis J., Tarantal, Alice F., Davidoff, Andrew M., and Nathwani, Amit C.

Subjects

*GENETIC transformation, *PERINATOLOGY, *HEMORRHAGE complications, *ADENO-associated virus, *HUMAN abnormalities, *LABORATORY mice, *POSTNATAL care, *PERIPHERAL vascular diseases

Abstract

We explored adeno-associated viral vector (AAV)-mediated gene transfer in the perinatal period in animal models of severe congenital factor VII (FVII) deficiency, a disease associated with early postnatal life-threatening hemorrhage. In young adult mice with plasma FVII < 1% of normal, a single tail vein administration of AAV (1 x 1013 vector genomes [vg]/kg) resulted in expression of murine FVII at 266% ± 34% of normal for ≥ 67 days, which mediated protection against fatal hemorrhage and significantly improved survival. Codon optimization of human FVII (hFVIIcoop) improved AAV transgene expression by 37-fold compared with the wild-type hFVII cDNA. In adult macaques, a single peripheral vein injection of 2 x 1011 vg/kg of the hFVIIcoop AAV vector resulted in therapeutic levels of hFVII expression that were equivalent in males (10.7% ± 3.1%) and females (12.3% ± 0.8%). In utero delivery of this vector in the third trimester to fetal monkeys conferred expression of hFVII at birth of 20.4% ± 3.7%, with a gradual decline to > 1% by 7 weeks. Re-administration of an alternative serotype at 12 months postnatal age increased hF-VII levels to 165% ± 6.2% of normal, which remained at therapeutic levels for a further 28 weeks without toxicity. Thus, pennatal AAV-mediated gene transfer shows promise for disorders with onset of pathology early after birth. (Blood. 2012; 119(4):957-966) [ABSTRACT FROM AUTHOR]

Published

2012

48. Inverse zonation of hepatocyte transduction with AAV vectors between mice and non-human primates

Author

Bell, Peter, Wang, Lili, Gao, Guangping, Haskins, Mark E., Tarantal, Alice F., McCarter, Robert J., Zhu, Yanqing, Yu, Hongwei, and Wilson, James M.

Subjects

*LIVER cells, *GENETIC transformation, *GENE therapy, *GENE expression, *GENETIC vectors, *ADENOVIRUS diseases, *LABORATORY mice

Abstract

Abstract: Gene transfer vectors based on adeno-associated virus 8 (AAV8) are highly efficient in liver transduction and can be easily administered by intravenous injection. In mice, AAV8 transduces predominantly hepatocytes near central veins and yields lower transduction levels in hepatocytes in periportal regions. This transduction bias has important implications for gene therapy that aims to correct metabolic liver enzymes because metabolic zonation along the porto-central axis requires the expression of therapeutic proteins within the zone where they are normally localized. In the present study we compared the expression pattern of AAV8 expressing green fluorescent protein (GFP) in liver between mice, dogs, and non-human primates. We confirmed the pericentral dominance in transgene expression in mice with AAV8 when the liver-specific thyroid hormone-binding globulin (TBG) promoter was used but also observed the same expression pattern with the ubiquitous chicken β-actin (CB) and cytomegalovirus (CMV) promoters, suggesting that transduction zonation is not caused by promoter specificity. Predominantly pericentral expression was also found in dogs injected with AAV8. In contrast, in cynomolgus and rhesus macaques the expression pattern from AAV vectors was reversed, i.e. transgene expression was most intense around portal areas and less intense or absent around central veins. Infant rhesus macaques as well as newborn mice injected with AAV8 however showed a random distribution of transgene expression with neither portal nor central transduction bias. Based on the data in monkeys, adult humans treated with AAV vectors are predicted to also express transgenes predominantly in periportal regions whereas infants are likely to show a uniform transduction pattern in liver. [Copyright &y& Elsevier]

Published

2011

49. AAV8-mediated Hepatic Gene Transfer in Infant Rhesus Monkeys (Macaca mulatta).

Author

Wang, Lili, Bell, Peter, Lin, Jianping, Calcedo, Roberto, Tarantal, Alice F, and Wilson, James M

Subjects

*GENETIC transformation, *NUCLEIC acids, *BILIARY tract, *BACTERIOPHAGES, *MICROBIAL genetics

Abstract

Many genetic metabolic diseases manifest in infancy, therefore, it is important to develop effective treatments that could be implemented at this time. Adeno-associated virus serotype 8 (AAV8) gene transfer has been studied in neonatal mouse, cat, and dog models and shown some efficacy with a single hepatic injection at birth. AAV8-mediated liver gene transfer has also generated sustained therapeutic effects in feline and canine models of lysosomal storage disorders. In these models, delaying the age of vector treatment increased gene transfer stability. The growth rate of infant nonhuman primates is more similar to the growth trajectory of humans, thus infant monkeys provide an excellent model to study AAV gene transfer efficiency, stability, and safety. In this study, we report for the first time that AAV8-mediated hepatic gene transfer in infant monkeys is safe and efficient but less stable when compared to adolescent animals. Infant monkeys administered AAV8 intravenously at 1 week postnatal age achieved up to 98% transduction of hepatocytes within 7 days of injection; however, there was significant dilution of genomes and loss of transgene expression 35 days postadministration. Delaying the injection to 1 month postnatal age did not improve stability of transduction but decreased the antibody response to AAV8 capsid. [ABSTRACT FROM AUTHOR]

Published

2011

50. Experimentally induced gestational androgen excess disrupts glucoregulation in rhesus monkey dams and their female offspring.

Author

Abbott, David H., Bruns, Cristin R., Barnett, Deborah K., Dunaif, Andrea, Goodfriend, Theodore L., Dumesic, Daniel A., and Tarantal, Alice F.

Abstract

Discrete fetal androgen excess during early gestation in rhesus monkeys (Macaca mulatta) promotes endocrine antecedents of adult polycystic ovary syndrome (PCOS)- like traits in female offspring. Because developmental changes promoting such PCOS-like metabolic dysfunction remain unclear, the present study examined time-mated, gravid rhesus monkeys with female fetuses, of which nine gravid females received 15 mg of testosterone propionate (TP) subcutaneously daily from 40 to 80 days (first to second trimesters) of gestation [term, mean (range): 165 (155-175) days], whereas an additional six such females received oil vehicle injections over the same time interval. During gestation, ultrasonography quantified fetal growth measures and was used as an adjunct for fetal blood collections. At term, all fetuses were delivered by cesarean section for postnatal studies. Blood samples were collected from dams and infants for glucose, insulin, and total free fatty acid (FFA) determinations. TP injections transiently accelerated maternal weight gain in dams, very modestly increased head diameter of prenatally androgenized (PA) fetuses, and modestly increased weight gain in infancy compared with concurrent controls. Mild to moderate glucose intolerance, with increased area-under-the-curve circulating insulin values, occurred in TP-injected dams during an intravenous glucose tolerance test in the early second trimester. Moreover, reduced circulating FFA levels occurred in PA fetuses during a third trimester intravenous glucagon-tolbutamide challenge (140 days gestation), whereas excessive insulin sensitivity and increased insulin secretion relative to insulin sensitivity occurred in PA infants during an intravenous glucose-tolbutamide test at ~1.5 mo postnatal age. Data from these studies suggest that experimentally induced fetal androgen excess may result in transient hyperglycemic episodes in the intrauterine environment that are sufficient to induce relative increases in pancreatic function in PA infants, suggesting in this nonhuman primate model that differential programming of insulin action and secretion may precede adult metabolic dysfunction [ABSTRACT FROM AUTHOR]

Published

2010