32 results on '"Soeiro R"'
Search Results
2. The Effects of Methionine Deprivation on Ribosome Synthesis in Hela Cells
- Author
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Vaughan, M. H., Soeiro, R., Warner, J. R., and Darnell, J. E.
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- 1967
3. The Turnover of Nuclear DNA-like RNA in HeLa Cells
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Soeiro, R., Vaughan, M. H., Warner, J. R., and Darnell,, J. E.
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- 1968
4. The Effect of Puromycin on Intranuclear Steps in Ribosome Biosynthesis
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Soeiro, R., Vaughan, M. H., and Darnell, J. E.
- Published
- 1968
5. Saccharomyces cerevisiae as a toxicological model to study synthetic cannabinoids and its pyrolysis products
- Author
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Ferreira, C., Couceiro, J., Soeiro, R., Noronha, J., Santos, C., Outeiro, T., Tenreiro, S., and Quintas, A.
- Subjects
Synthetic cannabinoids ,Saccharomyces cerevisiae - Abstract
Poster presented at the 7th European Academy of Forensic Science Conference. Prague, 6-11 September 2015 "Synthetic cannabinoids are among the major psychoactive drugs widespread as safe and legal alternatives to cannabis. They are commercially available as herbal incense products intended for smoke. This has led most of developed countries to concentrate efforts in order to ban the so called “legal highs”. Despite of their increasing use, there is still a lack of information on both synthetic and natural ingredients, pharmacokinetic properties and toxic effects. In fact some of the substances seem to have stronger toxicological effects when compared to their legal counterpart. Toxicological assays are paramount to know how harmful these new substances are, helping increase public awareness since several hospitalization cases have been reported due to consumption. To tackle the new challenges posed by novel drugs worldwide, we developed an approach using Saccharomyces cerevisiae as a model to investigate the toxicity of pyrolysis products of synthetic cannabinoids. S. cerevisiae."
- Published
- 2015
6. Neurosyphilis Presenting as Herpes Simplex Encephalitis
- Author
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Szilak, I., primary, Marty, F., additional, Helft, J., additional, and Soeiro, R., additional
- Published
- 2001
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7. Alterations in Human Fetal Hematopoiesis Are Associated with Maternal HIV Infection
- Author
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Burstein, Y, primary, Rashbaum, W K, additional, Hatch, W C, additional, Calvelli, T, additional, Golodner, M, additional, Soeiro, R, additional, and Lyman, W D, additional
- Published
- 1992
- Full Text
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8. Instillation of Vancomycin into a Cerebrospinal Fluid Reservoir to Clear Infection: Pharmacokinetic Considerations
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Hirsch, B. E., primary, Amodio, M., additional, Einzig, A. I., additional, Halevy, R., additional, and Soeiro, R., additional
- Published
- 1991
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9. Fv-1 host restriction of Friend leukemia virus: analysis of unintegrated proviral DNA
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Chinsky, J and Soeiro, R
- Abstract
The murine gene Fv-1 predominantly controls the outcome of infection by murine ecotropic retroviruses. The inhibition of virus replication by the Fv-1 gene product has been determined to be at an early stage in virus replication. Mechanistically, its effect appears to be on the accumulation of unintegrated proviral DNA or its integration or both. We investigated the synthesis of unintegrated proviral DNA, using several clones of B-, N-, or NB-tropic Friend murine leukemia virus. Our results indicate that the accumulation of B-tropic proviral DNA in NIH cells may be inhibited at either the level of linear (form III) or covalently closed circular DNA (form I), depending upon the degree of restriction of the clone of virus used. We confirmed that there is an effect of the Fv-1 gene on the accumulation of form I DNA of either B- or N-tropic Friend murine leukemia virus. However, the decrease in infectious centers effected by the Fv-1 gene did not correlate quantitatively with the effect on form I proviral DNA produced by N-tropic Friend murine leukemia virus in nonpermissive cells. Lastly, we demonstrated in nonpermissively infected NIH cells that a rapidly migrating doublet of viral DNA is formed.
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- 1981
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10. Fv-1 host restriction of Friend leukemia virus: oligonucleotide analysis of host range variants
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Duttagupta, S and Soeiro, R
- Abstract
The Fv-1 murine gene controls predominantly the replication of leukemia viruses of murine cells. Forced passage by B-tropic Friend leukemia virus in the restrictive host cells (NIH, Fv-1n/n) results in viral progeny capable of replicating efficiently in murine cells of any Fv-1 type, which are denoted as NB-tropic virus. We have studied the RNase T1-resistant oligonucleotide pattern of a series of NB-tropic Friend virus isolates and have been able to show changes from the parental B-tropic virus which occur at the 5' end of the genome. Cloned NB-tropic virus falls into three classes, demonstrating either four, one, or no apparent changes in the genome. These results suggest the possibility that conversion to NB tropism occurs by a recombination mechanism but, since change to NB tropism can occur without any observable oligonucleotide alteration, they do not confirm that any single oligonucleotide is diagnostic of NB tropism.
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- 1981
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11. Host restriction of Friend Leukemia virus coat protein synthesis
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Ray, U, Soeiro, R, and Fields, B N
- Abstract
Fv-1 gene-mediated host restriction of Friend leukemia virus replication was investigated in terms of coat protein synthesis. By using the assay of pseudotype formation with vesicular stomatitis virus. it was shown that under restricting growth conditions the availablity of leukemia virus coat protein for pseudotype formation was decreased. These studies appear to eliminate a pure assembly defect as the mechanism of Fv-1 host restriction.
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- 1976
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12. Fate of input oncornavirion RNA--biological studies
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Sveda, M M, Fields, B N, and Soeiro, R
- Abstract
The fate of input Friend leukemia virus RNA was studied using labeled input virus. The appearance of nuclear RNA-DNA hybrid molecules and the apparent integration of input virion RNA with host cell DNA was studied using a series of inhibitors of DNA or protein synthesis, cell growth conditions, and an intercalating agent. Under all these conditions of infection, little to no viral-specific RNA-DNA hybrid molecules were formed. These data demonstrate that the formation of such RNA-DNA hybrid structures requires conditions of infection that allow provirus synthesis and integration. Furthermore, they suggest that at least a fraction of input virion RNA may transiently become integrated with host cell DNA.
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- 1976
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13. Host restriction of Friend leukemia virus: synthesis and integration of the provirus.
- Author
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Sveda, M M and Soeiro, R
- Abstract
Host restriction of exogenous infection by murine leukemia viruses is controlled in vitro predominantly by the murine Fv-1 locus. The mechanism of this host restriction was investigated by comparing the early events in the replication of N-tropic versus B-tropic Friend leukemia virus in NIH 3T3 cells. These cells, which are Fv-1nn in type, are permissive for the N-tropic strain, but nonpermissive for the B-tropic strain, which replicates permissively in Balb/c cells. We have studied the synthesis, intracellular location, and molecular form of virus-specific DNA early in replication by means of molecular hybridization with a virus-specific DNA probe. Our results suggest that in the permissive infection viral DNA rapidly becomes integrated with cellular DNA. However, in the nonpermissive infection, although almost equal amounts of both positive and negative strand viral DNA are synthesized, integration of the provirus does not occur.
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- 1976
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14. Fv-1 host cell restriction of friend leukemia virus: microinjection of unintegrated viral DNA
- Author
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Chinsky, J, Soeiro, R, and Kopchick, J
- Abstract
The murine gene Fv-1 has been shown to exert a major influence over the replication of ecotropic murine leukemia viruses. Studies of the replication of Friend murine leukemia virus have shown that the restriction of viral replication occurs intracellularly after the initiation of viral DNA synthesis. The precise mechanism of the block imposed by the Fv-1 gene product is not completely understood. Our studies of Fv-1 restrictive infection have shown a variable decrease in the accumulation of intracellular unintegrated form I viral DNA. Analysis by microinjection of the viral DNA formed in nonpermissively infected BALB/c cells indicates that this DNA is infectious. These studies indicate that the form I DNA accumulated in nonpermissively infected BALB/c cells contains the complete viral sequences necessary for the production of viral progeny, and therefore, they suggest that the Fv-1 host restrictive mechanism recognizes viral factors other than form I DNA alone. These results support the possibility that Fv-1 host restriction occurs after formation of infectious viral DNA, perhaps at the integration step itself.
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- 1984
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15. Studies with aphidicolin on the Fv-1 host restriction of Friend murine leukemia virus
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Chinsky, J and Soeiro, R
- Abstract
The murine gene Fv-1 exerts a major control over the replication of Friend murine leukemia virus (F-MuLV). An effect of the gene product has been determined to be at the level of accumulation and integration of viral DNA. Aphidicolin, an inhibitor of eucaryotic DNA polymerase alpha, was studied in murine cells infected either permissively or nonpermissively with regard to the Fv-1 genotype. Results indicated that inhibition of DNA polymerase alpha did not affect the accumulation of form III viral DNA in either permissive or nonpermissive cells. However, the normal accumulation of circular form I DNA in permissive cells was inhibited. The block in the accumulation of form I DNA resembled that occurring in some F-MuLV Fv-1-nonpermissive infections. Additionally, aphidicolin treatment resulted in the accumulation of novel low-molecular-weight viral DNA species, normally detectable in a nonpermissive infection of NIH cells with B-tropic F-MuLV. These data suggest that the Fv-1 gene product may interact with host DNA polymerase alpha to prevent viral replication.
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- 1982
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16. Host restriction of Friend leukemia virus: gag proteins of host range variants.
- Author
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Duttagupta, S and Soeiro, R
- Abstract
The host response to murine ecotropic leukemia viruses is mainly controlled by the mouse Fv-1 gene. This locus controls virus replication at an intracellular stage and prevents provirus integration. Biological studies suggest that the Fv-1 effector molecule recognizes at least one virion structural protein. We have produced host range variants of B-tropic Friend murine leukemia virus in order to study the primary structure of potential viral target proteins. Our results show that conversion of B-tropism to NB-tropism is associated with changes in the primary structure of three gag proteins--p15, p12, and p30. These results suggest that host range conversion is due to a recombinational event, presumably between the parental virus and an endogenous murine virus. They also open the possibility that p12 and p30 may be involved in host range restriction.
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- 1981
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17. Nascent ribosomes from HeLa cells.
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Warner, J R and Soeiro, R
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- 1967
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18. Colonization of Skin and Development of Peritonitis Due to Coagulase-Negative Staphylococci in Patients Undergoing Peritoneal Dialysis
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Eisenberg, E. S., primary, Ambalu, M., additional, Szylagi, G., additional, Aning, V., additional, and Soeiro, R., additional
- Published
- 1987
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19. Assessment of sexual and reproductive access and use of menstrual products among Venezuelan migrant adult women at the Brazilian-Venezuelan border.
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Rocha L, Soeiro R, Gomez N, Costa ML, Surita FG, and Bahamondes L
- Abstract
Objective: To describe the sociodemographic characteristics, access to sexual and reproductive health (SRH) care, including contraceptives and to assess menstrual poverty of migrant Venezuelan adult women of childbearing age at the northwestern border between Venezuela and Brazil., Methods: Cross-sectional study coordinated by the Department of Obstetrics and Gynecology, University of Campinas, Campinas, SP, Brazil, conducted in Boa Vista, Roraima between January 18 and 24, 2021. We invited women aged 18 to 49 years to participate. A semi-structured self-response questionnaire was applied. The survey covered issues relating to SRH services, knowledge, access, and use of SRH services for women. We also applied a questionnaire regarding access to and quality of hygiene kits and toilets, and an open-ended question on " what does menstruation mean to you" ? We excluded illiterate women and those with amenorrhea, those who had undergone hysterectomy or tubal ligation, and those with partners who had undergone vasectomy., Findings: The age (mean ± SD) of the 177 respondent women was 28 ± 6.8 years, 32.2% reported that they had more than three children, 38.4% referred at least one unplanned pregnancy, and 52.5% of the women indicated an intention to become pregnant in the near future. Furthermore, 40 (29.8%) women sought a healthcare service because they wanted a contraceptive method; among them, 16 did not receive the contraceptive that they chose, and 15 women wanted to use a contraceptive implant. Regarding menstrual poverty, 64 women stated that the menstrual hygiene products provided by humanitarian organizations were not enough for their needs, and 44 women claimed being unable to wash their hands anytime they wanted to., Conclusions: The vulnerabilities of this cohort of Venezuelan migrant women in Brazil who lived mainly out of the official shelters further increase when they struggle with no knowledge of how to access SRH services, lack of provision of LARC methods, risk of unplanned pregnancy, and inappropriate access to menstrual hygiene products and sanitary services. There are several challenges to be overcome to ensure SRH care for migrant women in Brazil., Competing Interests: The authors have declared that no competing interests exist., (© 2022 The Authors. Published by Elsevier Ltd.)
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- 2022
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20. Planning for Happenstance: Helping Students Optimize Unexpected Career Developments.
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Vo M, Dallaghan GB, Borges N, Gill AC, Good B, Gollehon N, Mehta JJ, Richards B, Richards R, Serelzic E, Tenney-Soeiro R, Winward J, and Balmer D
- Subjects
- Faculty, Humans, Mentors, Retrospective Studies, Education, Medical, Students, Medical
- Abstract
Introduction: Planning for and responding to happenstance is an important but rarely discussed part of the professional development of medical students. We noted this gap while conducting a study of career inflection points of 24 physicians who frequently mentioned how luck had shaped their unfolding careers. A review of the career counseling literature led us to a body of work known as Planned Happenstance Learning Theory (PHLT). PHLT focuses on the attitudes and skills to make happenstance a positive force in one's life. We found no reference to this work in the medical education literature and resolved to address this gap., Methods: We created resources for an interactive, 90-minute faculty development workshop. In the workshop, the facilitator used a PowerPoint presentation, vignettes of happenstance, a student testimonial, and a reflection worksheet. We presented and formally evaluated the workshop at three national meetings for health science educators., Results: Workshop participants, mostly faculty ( N = 45), consistently expressed positive regard for the workshop content, organization, and instructional methods, especially the opportunity for guided reflection. A retrospective pre/postevaluation revealed a meaningful increase in knowledge about PHLT attitudes and skills, as well as a commitment to use these skills in promoting professional development., Discussion: The skills and attitudes of PHLT are relevant to students' career development. A workshop designed to introduce PHLT skills and attitudes to faculty advisors and mentors can help prepare faculty to promote students' awareness and use of these attitudes and skills., (© 2021 Vo et al.)
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- 2021
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21. Influence of simulation on electronic health record use patterns among pediatric residents.
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Orenstein EW, Rasooly IR, Mai MV, Dziorny AC, Phillips W, Utidjian L, Luberti A, Posner J, Tenney-Soeiro R, and Bonafide CP
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- Hospitals, Pediatric, Humans, Patient Handoff, Philadelphia, Electronic Health Records statistics & numerical data, Internship and Residency, Medical Informatics education, Pediatrics education, Simulation Training
- Abstract
Objective: Electronic health record (EHR) simulation with realistic test patients has improved recognition of safety concerns in test environments. We assessed if simulation affects EHR use patterns in real clinical settings., Materials and Methods: We created a 1-hour educational intervention of a simulated admission for pediatric interns. Data visualization and information retrieval tools were introduced to facilitate recognition of the patient's clinical status. Using EHR audit logs, we assessed the frequency with which these tools were accessed by residents prior to simulation exposure (intervention group, pre-simulation), after simulation exposure (intervention group, post-simulation), and among residents who never participated in simulation (control group)., Results: From July 2015 to February 2017, 57 pediatric residents participated in a simulation and 82 did not. Residents were more likely to use the data visualization tool after simulation (73% in post-simulation weeks vs 47% of combined pre-simulation and control weeks, P <. 0001) as well as the information retrieval tool (85% vs 36%, P < .0001). After adjusting for residents' experiences measured in previously completed inpatient weeks of service, simulation remained a significant predictor of using the data visualization (OR 2.8, CI: 2.1-3.9) and information retrieval tools (OR 3.0, CI: 2.0-4.5). Tool use did not decrease in interrupted time-series analysis over a median of 19 (IQR: 8-32) weeks of post-simulation follow-up., Discussion: Simulation was associated with persistent changes to EHR use patterns among pediatric residents., Conclusion: EHR simulation is an effective educational method that can change participants' use patterns in real clinical settings.
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- 2018
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22. Maternofetal transmission of human immunodeficiency virus-1: the role of antibodies to the V3 primary neutralizing domain.
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Rubinstein A, Goldstein H, Calvelli T, Devash Y, Rubinstein R, Soeiro R, and Lyman W
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- Amino Acid Sequence, Antibody Affinity, Female, Fetus microbiology, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 immunology, HIV Infections complications, HIV Infections immunology, Humans, Infant, Newborn, Maternal-Fetal Exchange, Molecular Sequence Data, Neutralization Tests, Peptides chemistry, Peptides immunology, Pregnancy, HIV Antibodies blood, HIV Infections transmission, HIV-1 immunology, HIV-1 isolation & purification, Pregnancy Complications, Infectious immunology
- Abstract
The increase in the number of human immunodeficiency virus-1 (HIV-1)-infected children is a direct consequence of the heterosexual spread of the disease to women and the growing number of HIV-positive i.v. drug users. It is not known how the majority of infants born to HIV-1-infected women escape HIV-1 infection, and, for those infected, the timing of HIV-1 transmission has yet to be determined. In addition, the role of maternal antibodies in the prevention of HIV-1 transmission to the fetus is unclear. We have previously demonstrated a correlation between vertical transmission and the absence of high-affinity/avidity antibodies to a peptide, KRI-HIGPGRAFYT, which corresponds to a region of the primary neutralizing domain of the gp120 V3 loop of HIVMN (MN-PND). The present study examines the correlation between the presence of these high affinity antibodies in women completing a pregnancy or undergoing an elective abortion and the detection of HIV-1 infection in their aborted fetuses. In several instances, transmission occurred despite high-affinity antibodies to the MN-PND. We have, therefore, evaluated the reactivity of sera to different MN-PND variants. In one infant born to a mother with high-affinity/avidity antibodies to KRI-HIGPGRAFYT (classic MN-PND), the infected baby developed antibodies to an MN-PND variant peptide against which his mother did not mount a humoral immune response during pregnancy. This finding indicates that fetal infection with MN-PND escape mutants arising during pregnancy may occur during a period when the mother is serologically negative.
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- 1993
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23. Maternofetal transmission of AIDS: frequency of human immunodeficiency virus type 1 nucleic acid sequences in human fetal DNA.
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Soeiro R, Rubinstein A, Rashbaum WK, and Lyman WD
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- Female, Genome, Viral, Humans, Polymerase Chain Reaction, Pregnancy, Pregnancy Trimester, Second, Acquired Immunodeficiency Syndrome transmission, DNA, Viral analysis, Fetus microbiology, HIV-1 genetics, Pregnancy Complications, Infectious microbiology
- Abstract
Pediatric AIDS is increasing in frequency due to a rise in the number of human immunodeficiency virus type 1 (HIV-1)-infected women of childbearing age. Because outcome studies reveal that most children infected peripartum manifest HIV-1-related disease in the first year of life, intrauterine infection has been suspected. Fetal tissues from 23 second-trimester abortuses were examined. The presence of HIV-1 nucleic acid sequences was determined by the polymerase chain reaction and used to define infection of the fetus. By analysis of available tissues, 7 of 23 fetuses were infected, while control fetal tissue was negative. In situ hybridization for HIV-1 DNA showed that only 1 of 8 infected abortuses was positive, while all samples of noninfected tissues revealed no HIV-1 DNA. These studies indicate that maternofetal transmission of HIV-1 may occur in 30% of pregnancies (7/23) by the end of the second trimester.
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- 1992
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24. HIV-1 infection of human fetal thymocytes.
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Tanaka KE, Hatch WC, Kress Y, Soeiro R, Calvelli T, Rashbaum WK, Rubinstein A, and Lyman WD
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- Cells, Cultured, DNA, Viral analysis, Female, Flow Cytometry, Gestational Age, Giant Cells, HIV-1 genetics, HIV-1 ultrastructure, Humans, Immunohistochemistry, Lymphocyte Activation, Microscopy, Electron, Phenotype, Polymerase Chain Reaction, Pregnancy, T-Lymphocytes ultrastructure, Thymus Gland cytology, Thymus Gland ultrastructure, Virion ultrastructure, HIV-1 physiology, T-Lymphocytes microbiology, Thymus Gland embryology, Virion physiology
- Abstract
Some neonates with congenital human immunodeficiency virus type 1 (HIV-1) infection exhibit immune dysregulation. This suggests that fetal CD4+ cells, possibly thymocytes, may be infected during gestation. If thymocytes are infected, this may result in a disruption of T-cell differentiation. To examine this hypothesis, normal human fetal thymocytes were established in tissue culture, characterized, and then exposed to HIV-1. On initial isolation, fetal thymocytes were analyzed for phenotypic markers by flow cytometry and assessed for T-cell function by mitogen-stimulated thymidine incorporation. The thymocytes comprised greater than 70% double positive (CD4+, CD8+) cells and responded to T- but not to B-cell mitogens. Thereafter, thymocytes were incubated in either tissue culture medium containing infectious HIV-1 or in control (HIV-free) medium. Infection of fetal thymocytes was determined by light and electron microscopy in combination with immunocytochemistry, molecular hybridization, and an infectious cell center (ICC) assay. After 1 week in culture, the thymocytes exposed to HIV-1 were positive by immunocytochemistry for the HIV-1-associated protein gp41. In addition, the presence of HIV-1 DNA was detected by molecular hybridization confirming infection of these cells. The ICC assay demonstrated the production of infectious HIV-1 particles and budding of mature virions was observed by electron microscopy. These studies demonstrate that human fetal thymocytes can be infected with HIV-1 in vitro and that this infection results in production of infectious virions. These results support the hypothesis that vertical transmission of HIV-1 in vivo may result in the infection of fetal thymocytes, which may contribute to postnatal HIV-1-associated pathologic conditions.
- Published
- 1992
25. Studies of the etiology of Crohn's disease using athymic nude mice.
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Das KM, Valenzuela I, Williams SE, Soeiro R, Kadish AS, and Baum SG
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- Animals, B-Lymphocytes immunology, Crohn Disease immunology, Female, Fluorescent Antibody Technique, Hyperplasia, Immunoglobulin G immunology, Inclusion Bodies, Viral, Lymph Nodes pathology, Lymphoma immunology, Male, Mice, Mice, Nude, Microscopy, Electron, Neoplasms, Experimental etiology, Neoplasms, Experimental immunology, Retroviridae, Crohn Disease etiology, Lymphoma etiology
- Abstract
Following injection of Crohn's disease tissue filtrates, lymphomas and hyperplastic lymph nodes developed in 16% of athymic nude (nu/nu) mice; whereas only 4% of control nude mice developed lymphadenopathy (p less than 0.025). One hundred forty coded sera from 111 patients (Crohn's disease = 36, ulcerative colitis = 28, diarrheal and other controls = 47) were assayed by indirect immunofluorescence for immunoreactivity with the lymphomas and hyperplastic lymph nodes. Coded sections were examined by two observers and scored on a 0 to 3 + scale. Fifty-four percent of the sera from patients with Crohn's disease were reactive with the Crohn's disease induced lymphoma by this assay. Eighty percent of sera from patients with symptomatic Crohn's disease were positive, whereas 22% of sera from patients in remission were positive. Sixty-six percent of sera from patients with symptomatic Crohn's disease reacted against hyperplastic lymph nodes induced by Crohn's disease filtrates. In contrast, only one control serum (from a patient with ulcerative colitis) reacted with the lymphomas or hyperplastic lymph nodes. Lymphomas induced by other means or arising spontaneously did not show immunofluorescence with Crohn's disease or control sera. Electron microscopy revealed C-type viral particles in five lymphomas induced by Crohn's disease filtrates and in one control lymphoma, but not in five hyperplastic lymph nodes and five control lymph nodes. Absorption of Crohn's disease sera with control lymphoma or with murine leukemia virus infected fibroblasts did not diminish immunoreactivity, whereas similar absorption with lymphomas induced by Crohn's disease filtrates abolished the immunofluorescence. These studies indicate that Crohn's disease tissue, when injected into athymic nude mice, induces lymphoid hyperplasia and lymphomas that contain an antigen(s) recognized by Crohn's disease sera.
- Published
- 1983
26. Immediate tricuspid valve replacement for endocarditis. Indications and results.
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Stern HJ, Sisto DA, Strom JA, Soeiro R, Jones SR, and Frater RW
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- Acute Disease, Adult, Bioprosthesis, Endocarditis, Bacterial etiology, Follow-Up Studies, Heart Valve Prosthesis, Humans, Staphylococcal Infections etiology, Substance-Related Disorders complications, Endocarditis, Bacterial surgery, Staphylococcal Infections surgery, Tricuspid Valve surgery
- Abstract
Tricuspid valve excision for tricuspid endocarditis in addicts is recommended to avoid early reinfection, continued sepsis, and late reinfection because of the resumption of intravenous drug abuse. Valvectomy is allegedly well tolerated hemodynamically by some, but it leads to heart failure in at least a third of patients. In our experience in 10 addicts with staphylococcal endocarditis who had failed to respond to antibiotic therapy, tricuspid valve replacement allowed all 10 to leave the hospital free of infection and free of heart failure. Resumption of drug addiction in three led to septic death, but not necessarily to tricuspid reinfection. Two returned to jobs requiring a high level of physical labor and tolerated this without difficulty. We find no need to follow the practice of tricuspid valve excision for tricuspid endocarditis in addicts. Those who refrain from drug abuse are well served by valve replacement. Those who do not are doomed with or without a tricuspid valve.
- Published
- 1986
27. Fungal peritonitis in patients receiving peritoneal dialysis: experience with 11 patients and review of the literature.
- Author
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Eisenberg ES, Leviton I, and Soeiro R
- Subjects
- Adolescent, Adult, Antifungal Agents therapeutic use, Candidiasis diagnosis, Candidiasis drug therapy, Candidiasis etiology, Female, Humans, Kidney Failure, Chronic therapy, Male, Middle Aged, Mycoses diagnosis, Mycoses drug therapy, Peritoneal Dialysis, Continuous Ambulatory adverse effects, Peritonitis diagnosis, Peritonitis drug therapy, Risk, Mycoses etiology, Peritoneal Dialysis adverse effects, Peritonitis etiology
- Abstract
Despite progress in decreasing the incidence of and improving the therapy for bacterial peritonitis in patients receiving peritoneal dialysis, fungal peritonitis has emerged as a relatively common infection. Hospitalization, recent prior episodes of peritonitis, and antibacterial therapy appear to predispose patients to this infection. Clinically, fungal peritonitis cannot be differentiated from bacterial peritonitis except by gram stain and culture of the dialysate. The most commonly made serious error is the failure to initiate appropriate therapy quickly enough on the basis of these diagnostic parameters. For patients who no longer require dialysis, those for whom a change to hemodialysis is preferred, and those with concomitant life-threatening illness, the recommended therapy for fungal peritonitis is removal of the dialysis catheter and the institution of therapy with systemic antifungal agents. For patients who are hemodynamically and metabolically stable and for whom continued peritoneal dialysis is desirable, a trial of antifungal chemotherapy before removal of the catheter may be indicated.
- Published
- 1986
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28. Proliferative membranopathy and human immunodeficiency virus in AIDS hearts.
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Flomenbaum M, Soeiro R, Udem SA, Kress Y, and Factor SM
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- Acquired Immunodeficiency Syndrome microbiology, Adult, Blotting, Southern, Cardiomyopathies microbiology, Cardiomyopathies pathology, DNA, Viral analysis, HIV Core Protein p24, HIV Envelope Protein gp120, HIV-1 genetics, Humans, Male, Mitochondria, Heart ultrastructure, Retroviridae Proteins analysis, Acquired Immunodeficiency Syndrome complications, Cardiomyopathies complications, HIV-1 isolation & purification, Heart microbiology, Myocardium ultrastructure
- Abstract
In order to determine if cardiac tissue from AIDS patients or patients with seropositivity to HIV-1 might be infected by HIV-1, portions of myocardium obtained postmortem were evaluated for HIV-1 DNA sequences. Cellular DNA was extracted and digested with EcoR1 and Southern blots were performed. One of three AIDS hearts was positive for HIV-1 DNA sequences without amplification, whereas two additional hearts were positive for HIV-1 DNA after amplification. Accordingly, other tissue from the heart positive for HIV-1 without amplification was studied by electron microscopy to localize HIV virions. Unexpectedly, large numbers of proliferating multilamellated membrane bodies were identified in myocytes, predominantly associated with mitochondria. Identical membrane bodies were found in two additional AIDS hearts, and in one heart from a patient with seropositivity to the AIDS virus, but in none of three similarly fixed controls. Immunocytochemistry for HIV core (p24) and envelope (gp120) antigens did not localize gold-labeled antibodies to the membrane bodies. We believe this membranopathy may be an HIV-1- or AIDS-specific abnormality of unknown etiology that may be related to the ultimate development of cardiomyopathy. In addition, our studies provide further support that HIV-1 may be present in AIDS hearts, although as yet we cannot state with certainty where the HIV-1 is located in these tissues.
- Published
- 1989
29. Arrested protein synthesis in polysomes of cultured chick embryo cells.
- Author
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Soeiro R and Amos H
- Subjects
- Animals, Carbon Isotopes, Chick Embryo, Blood, Culture Media, Dactinomycin pharmacology, Leucine metabolism, Microsomes metabolism, Protein Biosynthesis, RNA biosynthesis, Uracil Nucleotides pharmacology, Uridine metabolism
- Abstract
Cells deprived of serum synthesize proteins at a reduced rate; when serum is restored the rate returns to normal. The polysomes do not dissociate, but show reduced incorporation of amino acid in vitro, and are less responsive to polyuridylic acid than are those from normal cells.
- Published
- 1966
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30. A comparison between heterogeneous nuclear RNA and polysomal messenger RNA in HeLa cells by RNA-DNA hybridization.
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Soeiro R and Darnell JE
- Subjects
- Centrifugation, Density Gradient, History, 19th Century, Methods, Time Factors, Tritium, Cell Nucleus analysis, DNA, Neoplasm, HeLa Cells cytology, Hybridization, Genetic, RNA, Messenger analysis, RNA, Neoplasm analysis
- Abstract
Heterogeneous nuclear RNA (HnRNA) and mRNA from cytoplasmic polyribosomes of HeLa cells have been compared by RNA-DNA hybridization tests. 1 microg of HeLa cell DNA binds 0.05-0.10 microg of either HnRNA or mRNA. In addition, HeLa DNA that is preexposed to unlabeled HnRNA was found to have a reduced capacity to bind either HnRNA or mRNA. The results are compatible with considerable sequence similarity in the two types of RNA but, as is discussed, firm conclusions are precluded by imperfections of the hybridization reaction as presently employed.
- Published
- 1970
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31. Purification of oncornaviruses by agglutination with concanacalin A (murine leukemia virus-phytohemagglutinin-friend virus).
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Stewart ML, Summers DF, Soeiro R, Fields BN, and Maizel JV Jr
- Subjects
- Animals, Cells, Cultured, Centrifugation, Density Gradient, Concanavalin A pharmacology, Culture Media, Friend murine leukemia virus analysis, Friend murine leukemia virus growth & development, Friend murine leukemia virus pathogenicity, Glycoproteins analysis, Isotope Labeling, Methods, Mice, Mice, Inbred Strains, Microscopy, Electron, Sucrose, Tritium, Uridine metabolism, Viral Plaque Assay, Agglutination, Friend murine leukemia virus isolation & purification, Lectins pharmacology
- Abstract
Concanavalin A (Con A) has been used to rapidly and selectively agglutinate murine and avian oncornavirions from culture medium or plasma. The agglutinated virus was concentrated rapidly and gently by low-speed centrifugation and solubilization with alpha-methyl mannoside. Infectious virus was purified 2.3 times with respect to nucleic-acid content, and more than 60% of its infectivity was recovered. Infectious particles of densities 1.18 and 1.16 g/cm(3) were found in mouse cells infected with Friend virus. Con A reacted only with particles of density 1.16 g/cm(3), indicating heterogeneity with respect to carbohydrate content or structure as well as buoyant density. Electron microscopy of virus agglutinated with Con A showed a zone of Con A-glycoprotein complexes averaging 12-15 nm in thickness.
- Published
- 1973
- Full Text
- View/download PDF
32. Host restriction of Friend leukemia virus. Role of the viral outer coat.
- Author
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Krontiris TG, Soeiro R, and Fields BN
- Subjects
- Animals, Cell Line, Embryo, Mammalian, Friend murine leukemia virus drug effects, Immune Sera pharmacology, Mice, Mice, Inbred BALB C, Phenotype, Vesicular stomatitis Indiana virus drug effects, Viral Plaque Assay, Friend murine leukemia virus growth & development, Genes, Viral Proteins, Virus Replication
- Abstract
Host restriction of oncogenesis of RNA tumor viruses in vivo is associated with several gene loci. One of these genes, the Fv-1 locus in mice, is expressed in vitro and may be studied in mouse-embryo cultures that are restrictive or permissive for replication of Friend leukemia virus. Two strains of Friend leukemia virus, N-or B-tropic, show reciprocal ability to replicate successfully in either NIH Swiss (N-type) or BALB/c (B-type) cells that differ at the Fv-1 locus. These two strains of virus and two cell lines form a system to measure host restriction in vitro. Measurement of adsorption of Friend leukemia virus to permissive or restrictive cells reveals no difference in rate or total amount of virus bound. Furthermore, studies with virions of vesicular stomatitis virus phenotypically mixed within an envelope containing Friend leukemia virus protein show no differences in penetration or replication of vesicular stomatitis virus. These results strongly suggest that host restriction of Friend leukemia virus is due to an intracellular event in the viral replication cycle.
- Published
- 1973
- Full Text
- View/download PDF
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