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1. Collaborative Brazilian Pediatric Renal Transplant Registry (CoBrazPed-RTx): A Report From 2004 to 2013

Author

Garcia, C., Pestana, J.M., Martins, S., Nogueira, P., Barros, V., Rohde, R., Camargo, M., Feltran, L., Esmeraldo, R., Carvalho, R., Schvartsman, B., Vaisbich, M., Watanabe, A., Cunha, M., Meneses, R., Prates, L., Belangero, V., Palma, L., Carvalho, D., Matuk, T., Benini, V., Laranjo, S., Abbud-Filho, M., Charpiot, I.M.M., Ramalho, H.J., Lima, E., Penido, J., Andrade, C., Gesteira, M., Tavares, M., Penido, M., De Souza, V., and Wagner, M.

Published
2015
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2. Medico-social Aspects

Author

Paris, W. D., Thompson, S. E., Brawner, N. J., Penido, M. L., Bright, M. J., Robertson, C. M., Cooper, David K. C., editor, Miller, Leslie W., editor, and Patterson, G. Alexander, editor

Published
1996
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4. Latin-America Pediatric Renal Transplant Registry: 2004-2012 Report.: Abstract# A359

Author

Garcia, Druck C., Delucchi, A., Orta, N., Pestana, Medina J., Koch, P., Martins, S., Bittencourt, V., Rohde, R., Monteverde, M., Chaparro, A., Feltran, L., Camargo, M., Cunha, M., Shvartsman, B., Veisbich, M., Gesteira, F., Andrade, C., Esmeraldo, R., Carvalho, R., Oliveira, M., Ramalho, H., Fernandes, I., Prates, L., Palma, L., Belangero, V., Benini, V., Laranjo, S., Lima, E., Penido, J., Penido, M., Tavares, M., Ferraris, J., Hevia, P., Rosati, P., Repetto, H., Exeni, R., Florin, J., Casadei, D., Mellendez, K., Palacio, D., Madrigal, G., Sandoval, M., Loza, R., Jimenez, W., Galvez, H., Rodriguez, L., Puelma, F., Troche, A., Reyes, E., Marmol, A., Giron, F., Arteaga, B., Montoya, E., Martinez-Pico, M., Higueras, W., Liendo, C., Restrepo, J., Calcedo, L., Socorro, F., Semprum, P., Medeiros, M., Bosque, M., Serna, L., Salas, P., Coronel, V., Cisneros, A., Arriaga, J., Gastelbondo, R., Medjia, N., and Abbud-Filho, M.

Published
2014

5. Collaborative Brazilian Pediatric Renal Transplant Registry: 2004-2012.: Abstract# A478

Author

Garcia, C., Pestana, Medina J., Martins, S., Koch, P., Bittencourt, V., Rohde, R., Feltran, L., Camargo, M., Cunha, M., Esmeraldo, R., Carvalho, R., Prates, L., Belangero, V., Palma, L., Lima, E., Penido, J., Tavares, M., Penido, M., Gesteira, F., Andrade, C., Benini, V., Laranjo, S., Carvalho, D., Fernandes, I., Ramalho, H., Abbud-Filho, M., Oliveira, M., De Souza, V., Veisbich, M., Schvartsman, B., and Matuck, T.

Published
2014

8. Latin-America Pediatric Renal Transplant Registry: 2004-2012 Report.

Author

Garcia, Druck C., primary, Delucchi, A., additional, Orta, N., additional, Pestana, Medina J., additional, Koch, P., additional, Martins, S., additional, Bittencourt, V., additional, Rohde, R., additional, Monteverde, M., additional, Chaparro, A., additional, Feltran, L., additional, Camargo, M., additional, Cunha, M., additional, Shvartsman, B., additional, Veisbich, M., additional, Gesteira, F., additional, Andrade, C., additional, Esmeraldo, R., additional, Carvalho, R., additional, Oliveira, M., additional, Ramalho, H., additional, Fernandes, I., additional, Prates, L., additional, Palma, L., additional, Belangero, V., additional, Benini, V., additional, Laranjo, S., additional, Lima, E., additional, Penido, J., additional, Penido, M., additional, Tavares, M., additional, Ferraris, J., additional, Hevia, P., additional, Rosati, P., additional, Repetto, H., additional, Exeni, R., additional, Florin, J., additional, Casadei, D., additional, Mellendez, K., additional, Palacio, D., additional, Madrigal, G., additional, Sandoval, M., additional, Loza, R., additional, Jimenez, W., additional, Galvez, H., additional, Rodriguez, L., additional, Puelma, F., additional, Troche, A., additional, Reyes, E., additional, Marmol, A., additional, Giron, F., additional, Arteaga, B., additional, Montoya, E., additional, Martinez-Pico, M., additional, Higueras, W., additional, Liendo, C., additional, Restrepo, J., additional, Calcedo, L., additional, Socorro, F., additional, Semprum, P., additional, Medeiros, M., additional, Bosque, M., additional, Serna, L., additional, Salas, P., additional, Coronel, V., additional, Cisneros, A., additional, Arriaga, J., additional, Gastelbondo, R., additional, Medjia, N., additional, and Abbud-Filho, M., additional

Published
2014
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9. Collaborative Brazilian Pediatric Renal Transplant Registry: 2004-2012.

Author

Garcia, C., primary, Pestana, Medina J., additional, Martins, S., additional, Koch, P., additional, Bittencourt, V., additional, Rohde, R., additional, Feltran, L., additional, Camargo, M., additional, Cunha, M., additional, Esmeraldo, R., additional, Carvalho, R., additional, Prates, L., additional, Belangero, V., additional, Palma, L., additional, Lima, E., additional, Penido, J., additional, Tavares, M., additional, Penido, M., additional, Gesteira, F., additional, Andrade, C., additional, Benini, V., additional, Laranjo, S., additional, Carvalho, D., additional, Fernandes, I., additional, Ramalho, H., additional, Abbud-Filho, M., additional, Oliveira, M., additional, De Souza, V., additional, Veisbich, M., additional, Schvartsman, B., additional, and Matuck, T., additional

Published
2014
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10. Management of Fluid Status in Haemodialysis Patients: The Roles of Technology and Dietary Advice, Technical Problems in Patients on Hemodialysis

Author

Goretti Penido, M, Gardiner, C, Lindley, E, Aspinall, L, Garthwaite, E, Goretti Penido, M, Gardiner, C, Lindley, E, Aspinall, L, and Garthwaite, E

Abstract

The kidneys play a vital role in maintaining normal tissue hydration and serum sodium level. In haemodialysis patients, with impaired or absent kidney function, fluid status is managed by removing excess fluid using ultrafiltration and by restricting dietary sodium intake. Ideally, haemodialysis patients should remain close to normal hydration throughout the interdialytic period, with minimal periods of excessive dehydration or fluid overload and with no fluid–related co-morbidity. Optimal fluid management is achieved by adjusting the post-dialysis ‘target’ weight and, where necessary, limiting the fluid gained between dialysis sessions. While clinical history and examination remain the basis for prescribing the target weight, technology can provide useful objective information especially where the clinical indications are ambiguous. A simple non-invasive test can now be carried out when a patient attends for dialysis enabling staff to pick up changes in body composition so that their target weight can be adjusted to maintain optimal fluid status. In most patients, interdialytic fluid gain (IDFG) is directly related to sodium intake. Acceptable fluid gains can usually be achieved by limiting salt intake to the recommended daily allowance for the general population and avoiding unnecessary sodium loading during dialysis. Low pre-dialysis serum sodium levels can help identify patients with other causes of high IDFG, such as high blood sugar or social drinking, who need additional counselling. For the patients, lowering sodium intake may also improve blood pressure control and reduce requirements for antihypertensive medication. Staff education, and preferably participation, is vital when implementing salt restriction in a haemodialysis unit.

Published
2011

14. Medico-social Aspects.

Author

Cooper, David K. C., Miller, Leslie W., Patterson, G. Alexander, Paris, W. D., Thompson, S. E., Brawner, N. J., Penido, M. L., Bright, M. J., and Robertson, C. M.

Abstract

With the introduction of cyclosporin a new era in transplantation began. Improved immunosuppression was partly responsible for the exponential growth of heart transplant programs from 1984 to 1987[1]. The first successful lung transplant was performed by the Toronto Lung Transplant Croup in 1983 and, though less dramatic. there has been a steady increase in the number of lung transplant programs since that time[2]. More importantly. the increased frequency of organ transplantation has been accompanied by improved long-term survival. At the five heart and lung transplant programs represented by the authors of this chapter we found combined 1- and 5-year survival rates for heart (n=654) transplantation to be 89% and 75%. and for lung (n=196) transplantation to be 67% and 38%, respectively. [ABSTRACT FROM AUTHOR]

Published
1996
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15. ATP diphosphohydrolase from <e1>Schistosoma mansoni</e1> egg: characterization and immunocytochemical localization of a new antigen

Author

FARIA-PINTO, P., MEIRELLES, M. N. L., LENZI, H. L., MOTA, E. M., PENIDO, M. L. O., and COELHO, P. M. Z.

Abstract

The fact that the Schistosoma mansoni egg has two ATP diphosphohydrolase (EC 3.6.1.5) isoforms with different net charges and an identical molecular weight of 63000, identified by non-denaturing polyacrylamide gel electrophoresis and immunological cross-reactivity with potato apyrase antibodies, is shown. In soluble egg antigen (SEA), only the isoform with the lower net negative charge was detected and seemed to be the predominant species in this preparation. By confocal fluorescence microscopy, using anti-potato apyrase antibodies, the S. mansoni egg ATP diphosphohydrolase was detected on the external surface of miracidium and in von Lichtenberg's envelope. Intense fluorescence was also seen in the outer side of the egg-shell, entrapped by the surface microspines, suggesting that a soluble isoform is secreted. ATP diphosphohydrolase antigenicity was tested using the vegetable protein as antigen. The purified potato apyrase was recognized in Western blots by antibodies present in sera from experimentally S. mansoni-infected mice. In addition, high levels of IgG anti-ATP diphosphohydrolase antibodies were detected by ELISA in the same sera. This work represents the first demonstration of antigenic properties of S. mansoni ATP diphosphohydrolase and immunological cross-reactivity between potato apyrase and sera from infected individuals.

Published
2004

16. Psychosocial Issues in Heart Transplantation: A Review for Transplant Coordinators

Author

Paris, W, Brawner, N, Thompson, S, and Penido, M

Abstract

The latest advances in medicine and technology are used to care for transplant recipients, yet many patients have psychosocial difficulties that technology alone cannot resolve. Although most healthcare professionals acknowledge the importance of the staff's role in working with patients to resolve psychosocial problems, little research has examined the nature of staff-patient relationships and the proven ability of good relationships to improve outcomes. The purposes of this paper are to profile psychosocial risk and its relationship to outcomes after heart transplantation, explore staff-patient interactions in dealing with psychosocial problems, and present a growth and development model that can be used as a theoretical base to establish a more therapeutic alliance with patients.

Published
1997
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19. Management of Fluid Status in Haemodialysis Patients: The Roles of Technology and Dietary Advice, Technical Problems in Patients on Hemodialysis

Author

Gardiner, C, Lindley, E, Aspinall, L, Garthwaite, E, and Goretti Penido, M

Abstract

The kidneys play a vital role in maintaining normal tissue hydration and serum sodium level. In haemodialysis patients, with impaired or absent kidney function, fluid status is managed by removing excess fluid using ultrafiltration and by restricting dietary sodium intake. Ideally, haemodialysis patients should remain close to normal hydration throughout the interdialytic period, with minimal periods of excessive dehydration or fluid overload and with no fluid–related co-morbidity. Optimal fluid management is achieved by adjusting the post-dialysis ‘target’ weight and, where necessary, limiting the fluid gained between dialysis sessions. While clinical history and examination remain the basis for prescribing the target weight, technology can provide useful objective information especially where the clinical indications are ambiguous. A simple non-invasive test can now be carried out when a patient attends for dialysis enabling staff to pick up changes in body composition so that their target weight can be adjusted to maintain optimal fluid status. In most patients, interdialytic fluid gain (IDFG) is directly related to sodium intake. Acceptable fluid gains can usually be achieved by limiting salt intake to the recommended daily allowance for the general population and avoiding unnecessary sodium loading during dialysis. Low pre-dialysis serum sodium levels can help identify patients with other causes of high IDFG, such as high blood sugar or social drinking, who need additional counselling. For the patients, lowering sodium intake may also improve blood pressure control and reduce requirements for antihypertensive medication. Staff education, and preferably participation, is vital when implementing salt restriction in a haemodialysis unit.

Published
2011

20. Does Disclosure of Terminal Prognosis Mean Losing Hope? Insights from Exploring Patient Perspectives on Their Experience of Palliative Care Consultations.

Author

Coulourides Kogan A, Penido M, and Enguidanos S

Subjects
Female, Hospitals, Community, Humans, Inpatients psychology, Interviews as Topic, Los Angeles, Male, Middle Aged, Prognosis, Qualitative Research, Referral and Consultation, Caregivers psychology, Disclosure, Hope, Palliative Care psychology, Terminally Ill psychology
Abstract

Background: A primary barrier to physician disclosure of terminal prognosis is concern that patients will lose hope. Inpatient palliative care (IPC) teams are especially posed to mediate this barrier, but little is known about patient perceptions and experience of IPC., Objective: This study aimed to elicit seriously ill patients' perspective and experience of an IPC consultation, and to explore patient attitudes toward information derived from the consultation., Methods: An exploratory, qualitative study was conducted at a large nonprofit community hospital in the Los Angeles area. An established IPC team conducted individualized consults with patients and families within 24 hours of referral. Eligible participants were English-speaking adults, aged 18 or over, who had received an IPC consultation within the previous week during their hospitalization. Purposive recruitment of patients was conducted by the IPC social worker. Interviews were conducted at bedside using a semistructured interview protocol employing open-ended questions., Results: Twelve seriously ill patients were interviewed. Four themes were identified from the interview transcripts: (1) holistic care approach, (2) knowledge/information gained, (3) hope and enlightenment, and (4) patient readiness., Conclusions: Results suggest that disclosure of a terminal prognosis does not mean loss of patient hope. Instead, hope was redefined on a goal other than cure. Presenting patients with information and increasing their knowledge about care options and resources may facilitate patients in identifying meaningful goals that are better aligned with their prognosis.

Published
2015
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21. Family members' perceptions of inpatient palliative care consult services: a qualitative study.

Author

Enguidanos S, Housen P, Penido M, Mejia B, and Miller JA

Subjects
Adult, Aged, Chronic Disease therapy, Communication, Conflict, Psychological, Female, Humans, Interviews as Topic, Male, Middle Aged, Patient Care Team standards, Qualitative Research, Referral and Consultation statistics & numerical data, Severity of Illness Index, Terminal Care psychology, United States, Young Adult, Decision Making, Family psychology, Palliative Care methods, Professional-Family Relations, Referral and Consultation standards
Abstract

Background: Family members are commonly involved in end-of-life decision making and typically involved in inpatient palliative care consultations. Although much research has documented patient outcomes following inpatient palliative care consultation, little is known about family member perceptions of the consultation., Aim: The purpose of this study was to determine how inpatient palliative care consultations impacted family members' understanding of the patient's condition, knowledge of available care options, and decision-making ability., Design: An exploratory, qualitative study was conducted employing individual interviews among family members of seriously ill patients, recruited purposively. Interviews were conducted in person, at the hospital, or via telephone, using a semistructured protocol., Setting/participants: Family members of seriously ill patients were recruited from a nonprofit, community hospital., Results: Interviews were conducted among 23 family members. Four themes were identified and included: perceived qualities of the inpatient palliative care consultation, family readiness, impact on decision-making process, and focus on comfort and quality of life. While most comments reflected positive aspects of the inpatient palliative care consult, such as improved pain control and communication, and increased access to medical professionals and time to discuss patient conditions, some themes reflected a lack of adequate preparation for the inpatient palliative care consultation and readiness for discussing prognosis., Conclusion: Family members report discussion with the inpatient palliative care team results in improved communication and knowledge, which contributes to decision-making ability. However, palliative care consultation may be improved by developing stronger protocols for introducing palliative care and by including the attending physician in the process to preclude conflicting, inconsistent information and recommendations.

Published
2014
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22. Phosphate homeostasis and its role in bone health.

Author

Goretti Penido M and Alon US

Subjects
Animals, Bone Diseases, Metabolic pathology, Bone Diseases, Metabolic physiopathology, Bone Remodeling, Bone and Bones pathology, Bone and Bones physiopathology, Calcitriol metabolism, Fibroblast Growth Factor-23, Fibroblast Growth Factors metabolism, Growth Plate metabolism, Homeostasis, Humans, Intestinal Absorption, Intestinal Mucosa metabolism, Kidney metabolism, Parathyroid Hormone metabolism, Signal Transduction, Bone Diseases, Metabolic metabolism, Bone and Bones metabolism, Phosphates metabolism
Abstract

Phosphate is one of the most abundant minerals in the body, and its serum levels are regulated by a complex set of processes occurring in the intestine, skeleton, and kidneys. The currently known main regulators of phosphate homeostasis include parathyroid hormone (PTH), calcitriol, and a number of peptides collectively known as the "phosphatonins" of which fibroblast growth factor-23 (FGF-23) has been best defined. Maintenance of extracellular and intracellular phosphate levels within a narrow range is important for many biological processes, including energy metabolism, cell signaling, regulation of protein synthesis, skeletal development, and bone integrity. The presence of adequate amounts of phosphate is critical for the process of apoptosis of mature chondrocytes in the growth plate. Without the presence of this mineral in high enough quantities, chondrocytes will not go into apoptosis, and the normal physiological chain of events that includes invasion of blood vessels and the generation of new bone will be blocked, resulting in rickets and delayed growth. In the rest of the skeleton, hypophosphatemia will result in osteomalacia due to an insufficient formation of hydroxyapatite. This review will address phosphate metabolism and its role in bone health.

Published
2012
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23. Improved canine and human visceral leishmaniasis immunodiagnosis using combinations of synthetic peptides in enzyme-linked immunosorbent assay.

Author

Costa MM, Penido M, dos Santos MS, Doro D, de Freitas E, Michalick MS, Grimaldi G, Gazzinelli RT, and Fernandes AP

Subjects
Animals, Brazil, Dogs, Enzyme-Linked Immunosorbent Assay methods, Humans, Immunologic Tests methods, Sensitivity and Specificity, Clinical Laboratory Techniques methods, Dog Diseases diagnosis, Leishmaniasis, Visceral diagnosis, Leishmaniasis, Visceral veterinary, Peptides
Abstract

Background: Zoonotic visceral leishmaniasis (VL) is a severe infectious disease caused by protozoan parasites of the genus Leishmania and the domestic dogs are the main urban parasite reservoir hosts. In Brazil, indirect fluorescence antibody tests (IFAT) and indirect enzyme linked immunosorbent assay (ELISA) using promastigote extracts are widely used in epidemiological surveys. However, their sensitivity and specificity have often been compromised by the use of complex mixtures of antigens, which reduces their accuracy allowing the maintenance of infected animals that favors transmission to humans. In this context, the use of combinations of defined peptides appears favorable. Therefore, they were tested by combinations of five peptides derived from the previously described Leishmania diagnostic antigens A2, NH, LACK and K39., Methodology/principal Findings: Combinations of peptides derived A2, NH, LACK and K39 antigens were used in ELISA with sera from 44 human patients and 106 dogs. Improved sensitivities and specificities, close to 100%, were obtained for both sera of patients and dogs. Moreover, high sensitivity and specificity were observed even for canine sera presenting low IFAT anti-Leishmania antibody titers or from asymptomatic animals., Conclusions/significance: The use of combinations of B cell predicted synthetic peptides derived from antigens A2, NH, LACK and K39 may provide an alternative for improved sensitivities and specificities for immunodiagnostic assays of VL.

Published
2012
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24. [The seroprevalence of HCV in patients submitted to hemodialysis and health professionals in the State of Minas Gerais, southwest of Brazil].

Author

Oliveira Penido JM, Caiaffa WT, Guimarães Penido M, Caetano EV, Carvalho AR, Leite AF, Faria SC, Gomide IV, Rosa AA, Penido MG, and Teixeira R

Subjects
Adolescent, Adult, Aged, Brazil, Child, Child, Preschool, Cross-Sectional Studies, Female, Humans, Infant, Male, Middle Aged, Seroepidemiologic Studies, Health Personnel, Hepatitis C blood, Hepatitis C epidemiology, Hepatitis C Antibodies blood, Kidney Failure, Chronic blood, Renal Dialysis
Abstract

Unlabelled: Patients with chronic renal failure(CRF) in hemodialysis(HD) programs comprise a risk group for acquisition of hepatitis C virus(HCV) infection. The objectives were to evaluate the seroprevalence of HCV in patients submitted to HD in State of Minas Gerais(MG), southwest of Brazil; to correlate this seroprevalence with the time of treatment on HD; to investigate the anti-HCV seropositivity in health professionals, to investigate the existence of a correlation between mean HCV seroprevalence and the human development index (HDI). Patients from 66 healthcare units(HU) were studied using a validated questionnaire and considering the positive values of anti-HCV(Elisa III) tests performed in these units between january and december 2003., Results: the majority of patients were male (56.2%), between 41 and 60 years old. The mean seroprevalence of HCV in the 66 healthcare units was 13+/-9.5%; the three-monthly seroprevalence was below 20%, 15% and 10% in 75%, 50% and 40% of healthcare units, respectively. When the HU were grouped according to HCV seroprevalence into low(<5%), medium(5-15%) and high seroprevalence(>15%), 20% of the units have low, 42% medium and 37.5% were found to have high seroprevalence. No correlation was found between HDI and HCV seroprevalence (r=0.42; p=0.174) but in the regions in which the HDI was higher, HCV seroprevalence was also higher. There was a positive correlation between HCV seroprevalence and time on HD in 884 patients in the 4 HU (p<0.001). The seroprevalence of HCV was investigated in 387 healthcare professionals(29%) working in 14 HU. They were divided into two groups according to their time of professional activity: <10 y (G1) and >10 y (G2). In G1, there were no cases of anti-HCV seropositivity. In G2, 3 members of the staff were anti-HCV seropositive. The mean time of work of the seropositive staff in the HU was 15.6 years. The seroprevalence of HCV was 0.8% when all the healthcare professionals were taken into consideration. There was no statistically significant difference with respect to HCV seroprevalence between G1 and G2 with respect to the time of occupational exposure (p=0.27)., Conclusion: the seroprevalence of HCV in patients on HD in MG is 13+/-9.5% and was <10% in 40% of the HU; there was no statistically significant correlation between HDI and seroprevalence of HCV in the healthcare units evaluated; there was a statistically significant correlation between HCV seroprevalence and time of treatment on HD; HCV seroprevalence in the health professionals studied was 0.8% and similar to the literature.

Published
2008

25. A new series of schistosomicide drugs, the alkylaminoalkanethiosulfuric acids, partially inhibit the activity of Schistosoma mansoni ATP diphosphohydrolase.

Author

Luiz Oliveira Penido M, Resende DM, Vianello MA, Humberto da Silveira Bordin F, Jacinto AA, Dias WD, Montesano MA, Nelson DL, Marcos Zech Coelho P, and Vasconcelos EG

Subjects
Adenosine Triphosphatases metabolism, Animals, Apyrase metabolism, Dithiothreitol pharmacology, Glutathione pharmacology, Iodoacetamide pharmacology, Male, Mice, Schistosoma mansoni enzymology, Solanum tuberosum enzymology, Sulfhydryl Reagents pharmacology, Apyrase antagonists & inhibitors, Schistosoma mansoni drug effects, Schistosomicides pharmacology, Sulfuric Acid Esters pharmacology
Abstract

The effects of the alkylaminoalkanethiosulfuric acids (AAATs), new schistosomicidal drugs, on Schistosoma mansoni ATP diphosphohydrolase isoforms, members of the NTPDase family, were analyzed. Pre-incubation of worm adult tegument with AAATs derivatives, with small apolar alkyl groups and an apolar alkane portion of 6 or 8 carbon atoms linked to the amino group, inhibited ATPase activity with a Ki 100-1000 microM. Little inhibition (20%) was observed when ADP was the substrate. The 2-[(tert-butyl)amino]-1-ethanethiosulfuric acid (100 microM) which has a less lipophilic structure, inhibited 28% ATPase and 12% ADPase activities, suggesting that the lipophilicity, although important, is not the only requisite for enzyme activity inhibition. The N-(sec-butyl)-2-bromo-1-octanaminium bromide, which contains a bromide atom instead of thiosulphate, inhibited <10% of the enzyme activity, suggesting the involvement of cysteine residue(s) from S. mansoni ATP diphosphohydrolase isoforms in a mixed disulfide formation. Treatment of parasite tegument with 5 mM iodoacetamide or 1 mM dithiothreitol protected ATPase and ADPase activities against inhibition by AAATs, corroborating the participation of disulfide interchange in the AAATs mechanism. Since S. mansoni ATP diphosphohydrolase isoforms and potato apyrase share structural similarities, the latter enzyme was also tested. ADPase activity from potato apyrase was inhibited by 55%, showing a higher sensitivity to 1 mM AAATs than that shown by ADPase activity from the tegument, while the ATPase activities from both samples showed similar inhibition levels. Furthermore, sulfhydryl reagents protected potato apyrase activity. Therefore, it is possible that both soluble S. mansoni ATP diphosphohydrolase and membrane-associated isoforms are targets for the AAATs.

Published
2007
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26. Cross-immunoreactivity between anti-potato apyrase antibodies and mammalian ATP diphosphohydrolases: potential use of the vegetal protein in experimental schistosomiasis.

Author

Faria-Pinto P, Meirelles MN, Lenzi HL, Mota EM, Penido ML, Coelho PM, and Vasconcelos EG

Subjects
Adenosine Triphosphatases metabolism, Amino Acid Sequence, Animals, Antibodies, Helminth immunology, Apyrase metabolism, Cross Reactions, Disease Models, Animal, Male, Mice, Microscopy, Confocal, Molecular Sequence Data, Rabbits, Schistosoma mansoni immunology, Schistosoma mansoni metabolism, Adenosine Triphosphatases immunology, Apyrase immunology, Schistosoma mansoni enzymology, Schistosomiasis mansoni immunology, Solanum tuberosum enzymology
Abstract

We have previously showed that Schistosoma mansoni ATP-diphosphohydrolase and Solanum tuberosum potato apyrase share epitopes and the vegetable protein has immunostimulatory properties. Here, it was verified the in situ cross-immunoreactivity between mice NTPDases and anti-potato apyrase antibodies produced in rabbits, using confocal microscopy. Liver samples were taken from Swiss Webster mouse 8 weeks after infection with S. mansoni cercariae, and anti-potato apyrase and TRITC-conjugated anti-rabbit IgG antibody were tested on cryostat sections. The results showed that S. mansoni egg ATP diphosphohydrolase isoforms, developed by anti-potato apyrase, are expressed in miracidial and egg structures, and not in granulomatous cells and hepatic structures (hepatocytes, bile ducts, and blood vessels). Therefore, purified potato apyrase when inoculated in rabbit generates polyclonal sera containing anti-apyrase antibodies that are capable of recognizing specifically S. mansoni ATP diphosphohydrolase epitopes, but not proteins from mammalian tissues, suggesting that autoantibodies are not induced during potato apyrase immunization. A phylogenetic tree obtained for the NTPDase family showed that potato apyrase had lower homology with mammalian NTPDases 1-4, 7, and 8. Further analysis of potato apyrase epitopes could implement their potential use in schistosomiasis experimental models.

Published
2006
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27. [Idiopathic hypercalciuria: presentation of 471 cases]

Author

Penido MG, Diniz JS, Moreira ML, Tupinambá AL, França A, Andrade BH, and Souto MF

Abstract

OBJECTIVE: To analyze the clinical history and evolution of children and adolescents with IH, emphasizing some of their peculiar features. METHODS: We followed 471 patients with IH at an outpatient clinic. Patients were submitted to the following protocol: abdominal X-ray, kidney and urinary tract ultrasonography; urinary ionogram, blood gas and biochemical analyses; 24-hour urine for measurement of calcium and other electrolytes and creatinine; urinalysis, urine culture and phase-contrast microscopy; second morning urine collected after fasting for measurement of calcium and creatinine. RESULTS: At the time of diagnosis, 6% of the patients were infants, 15% pre-school children, 55% school children, and 24% adolescents; 56% of them were boys. Clinical and laboratory findings were: 47% had hematuria and abdominal pain, 31% had isolated hematuria, 14% isolated abdominal pain, and 8% had urinary tract infection, nocturnal enuresis, suprapubic pain or urethralgia, or the frequency/urgency syndrome with urinary incontinence. Hypercalciuria was associated with urolithiasis in 56% of patients. There was association with hyperuricosuria in 18.5% of the cases, and hypocitraturia in 8.5% of the cases. Evolution was poor for 33% of the patients, with recurrence of nephrolithiasis, persistence of hematuria, and abdominal pain. CONCLUSIONS: IH must be diagnosed and treated with criteria in order to reduce consequences such as hematuria, abdominal pain, urinary stone formation and possible bone involvement. Signs and symptoms such as urgency and urinary incontinence, suprapubic pain and nocturnal enuresis may result from renal hyperexcretion of calcium.

Published
2001
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28. Schistosomicidal activity of alkylaminooctanethiosulfuric acids.

Author

Penido ML, Nelson DL, Vieira LQ, and Coelho PM

Subjects
Animals, Female, Male, Mice, Schistosoma mansoni metabolism, Schistosomicides chemistry, Sulfuric Acids administration & dosage, Schistosomiasis mansoni metabolism, Schistosomicides metabolism, Sulfuric Acids metabolism
Abstract

The schistosomicidal activity of a new series of alkylaminooctanethiosulfuric acids was studied in white Swiss mice infected with the L.E. strain of Schistosoma mansoni (Belo Horizonte, MG, Brazil). In a preliminary screening of six compounds, two derivatives - 2-[(1-methylpropyl)amino]-1-octanethiosulfuric acid and 2-[(1-methylethyl)-amino]-1-octanethiosulfuric acid - given orally in doses of 300 mg/kg/day for five consecutive days, caused interruption of the oviposition and the hepatic shift of more than 90% of the worms. Both compounds caused a significant reduction in worm burden and, interestingly, the female schistosomes were more susceptible. With the therapeutic schedule of two doses of 800 mg/kg over a 20 day interval, the death of almost all the females and about 50% of the males was observed. Female worms recovered from treated mice showed scattered vitteline glands. Results of in vitro experiments against different developmental stages of the parasite revealed the induction of paralysis and damage to the tegument membrane. The drugs presented no toxic effects on the animals.

Published
1994
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