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Introduction: Spinal cord injury (SCI) cause significant disability and impact the quality of life of those affected by it. The nutritional status and diet are fundamental to diminish the progression of complications; vitamins modulate the inflammatory response and oxidative stress, promote blood-spinal cord barrier preservation and the prompt recovery of homeostasis. A deep knowledge of the benefits achieved from vitamins in patients with SCI are summarized. Information of dosage, time, and effects of vitamins in these patients are also displayed. Vitamins have been extensively investigated; however, more clinical trials are needed to clarify the scope of vitamin supplementation.Objective: The objective of this review was to offer relevant therapeutic information based on vitamins supplementation for SCI patients.Methods: Basic and clinical studies that have implemented the use of vitamins in SCI were considered. They were selected from the year 2000-2022 from three databases: PubMed, Science Direct and Google Scholar.Results: Consistent benefits in clinical trials were shown in those who were supplemented with vitamin D (prevents osteoporosis and improves physical performance variables), B3 (improves lipid profile) and B12 (neurological prophylaxis of chronic SCI damage) mainly. On the other hand, improvement related to neuroprotection, damage modulation (vitamin A) and its prophylaxis were associated to B complex vitamins supplementation; the studies who reported positive results are displayed in this review.Discussion: Physicians should become familiar with relevant information that can support conventional treatment in patients with SCI, such as the use of vitamins, a viable option that can improve outcomes in patients with this condition.
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Traumatismos da Medula Espinal , Vitaminas , Humanos , Vitaminas/uso terapêutico , Vitamina A , Qualidade de Vida , Estresse Oxidativo/fisiologia , Traumatismos da Medula Espinal/complicações , Traumatismos da Medula Espinal/tratamento farmacológico , Vitamina K/uso terapêutico , Medula EspinalRESUMO
Plant breeders have indirectly selected for variation at circadian-associated loci in many of the world's major crops, when breeding to increase yield and improve crop performance. Using an eight-parent Multiparent Advanced Generation Inter-Cross (MAGIC) population, we investigated how variation in circadian clock-associated genes contributes to the regulation of heading date in UK and European winter wheat (Triticum aestivum) varieties. We identified homoeologues of EARLY FLOWERING 3 (ELF3) as candidates for the Earliness per se (Eps) D1 and B1 loci under field conditions. We then confirmed a single-nucleotide polymorphism within the coding region of TaELF3-B1 as a candidate polymorphism underlying the Eps-B1 locus. We found that a reported deletion at the Eps-D1 locus encompassing TaELF3-D1 is, instead, an allele that lies within an introgression region containing an inversion relative to the Chinese Spring D genome. Using Triticum turgidum cv. Kronos carrying loss-of-function alleles of TtELF3, we showed that ELF3 regulates heading, with loss of a single ELF3 homoeologue sufficient to alter heading date. These studies demonstrated that ELF3 forms part of the circadian oscillator; however, the loss of all homoeologues was required to affect circadian rhythms. Similarly, loss of functional LUX ARRHYTHMO (LUX) in T. aestivum, an orthologue of a protein partner of Arabidopsis (Arabidopsis thaliana) ELF3, severely disrupted circadian rhythms. ELF3 and LUX transcripts are not co-expressed at dusk, suggesting that the structure of the wheat circadian oscillator might differ from that of Arabidopsis. Our demonstration that alterations to ELF3 homoeologues can affect heading date separately from effects on the circadian oscillator suggests a role for ELF3 in cereal photoperiodic responses that could be selected for without pleiotropic deleterious alterations to circadian rhythms.
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Arabidopsis , Relógios Circadianos , Triticum/genética , Arabidopsis/genética , Melhoramento Vegetal , Ritmo Circadiano/genética , Relógios Circadianos/genética , Regulação da Expressão Gênica de PlantasRESUMO
Safeners are agrochemicals co-applied with herbicides that facilitate selective control of weeds by protecting monocot crops from chemical injury through enhancing the expression of detoxifying enzymes such as glutathione transferases (GSTs). Even though the application of safeners causes the induction of genes encoding GSTs in model dicots such as Arabidopsis thaliana, safeners do not protect broadleaf crops from herbicide injury. In this study, we proposed that the localized induction of Arabidopsis GSTs and the fundamental differences in their detoxifying activity between dicot and monocot species, underpin the failure of safeners to protect Arabidopsis from herbicide toxicity. Using the herbicide safener, isoxadifen-ethyl, we showed that three tau (U) family GSTs namely AtGSTU7, AtGSTU19 and AtGSTU24 were induced with different magnitude by isoxadifen treatment in root and rosette tissues. The higher magnitude of inducibility of these AtGSTUs in the root tissues coincided with the enhanced metabolism of flufenacet, a herbicide that is active in root tissue, protecting Arabidopsis plants from chemical injury. Assay of the recombinant enzyme activities and the significant reduction in flufenacet metabolism determined in the T-DNA insertion mutant of AtGSTU7 (gstu7) in Arabidopsis plants identified an important function for AtGSTU7 protein in flufenacet detoxification. In-silico structural modeling of AtGSTU7, suggested the unique high activity of this enzyme toward flufenacet was due to a less constrained active site compared to AtGSTU19 and AtGSTU24. We demonstrate here that it is possible to induce herbicide detoxification in dicotyledonous plants by safener treatment, albeit with this activity being restricted to very specific combinations of herbicide chemistry, and the localized induction of enzymes with specific detoxifying activities.
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Background: Research into public risk perceptions associated with emerging risks in agriculture and supply chains has focused on technological risks, zoonotic diseases, and food integrity, but infrequently on naturally occurring diseases in plants. Plant virus infections account for global economic losses estimated at $30 billion annually and are responsible for nearly 50% of plant diseases worldwide, threatening global food security. This research aimed to understand public perceptions of emerging risks and benefits associated with plant viruses in agriculture in Belgium, Slovenia, Spain, and the UK. Methods: Online qualitative semi-structured interviews with 80 European consumers were conducted, including 20 participants in each of Belgium, Slovenia, the UK, and Spain. Microsoft Streams was used to transcribe the interview data, and NVivo was utilized to code the transcripts and analyze the data. Results: The results indicate that, while study participants were relatively unfamiliar with the plant viruses and their potential impacts, plant viruses evoked perceived risks in a similar way to other emerging risks in the agri-food sector. These included risks to environment and human health, and the economic functioning of the relevant supply chain. Some participants perceived both risks and benefits to be associated with plant viruses. Benefits were perceived to be associated with improved plant resistance to viruses. Conclusions: The results provide the basis for risk regulation, policy, and communication developments. Risk communication needs to take account of both risk and benefit perceptions, as well as the observation that plant viruses are perceived as an emerging, rather than an established, understood, and controlled risk. Some participants indicated the need for risk-benefit communication strategies to be developed, including information about the impacts of the risks, and associated mitigation strategies. Participants perceived that responsibility for control of plant viruses should be conferred on actors within the supply chain, in particular primary producers, although policy support (for example, financial incentivization) should be provided to improve their motivation to instigate risk mitigation activities.
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Background: Osteocalcin plays a role in glucose metabolism in mice, but its relevance in human energetic metabolism is controversial. Its relationship with markers of energetic metabolism in the pediatric population has not been systematically addressed in infants and adolescents. Objective: This study aims to assess the mean differences between tOC, ucOC, and cOC among healthy children and children with type 1 or type 2 diabetes (T1D or T2D) and the correlation of these bone molecules with metabolic markers. Methods: A systematic review and metanalysis were performed following PRISMA criteria to identify relevant observational studies published in English and Spanish using PubMed, Scopus, EBSCO, and Web of Science databases. The risk of bias was assessed using New Castle-Ottawa scale. Effect size measures comprised standardized mean difference (SMD) and Pearson correlations. Heterogeneity and meta-regressions were performed. Results: The 20 studies included were of high quality and comprised 3,000 pediatric patients who underwent tOC, cOC, or ucOC measurements. Among healthy subjects, there was a positive correlation of ucOC with WC and weight, a positive correlation of tOC with FPG, HDL-c, WC, height, and weight, and a negative correlation between tOC and HbA1c. Among diabetic subjects, a negative correlation of ucOC with HbA1c and glycemia in both T1D and T2D was found and a negative correlation between tOC and HbA1c in T1D but not in T2D. The ucOC concentrations were lower in T2D, T1D, and patients with abnormal glucose status than among controls. The serum concentrations of tOC concentrations were lower among T1D than in controls. The patient's age, altitude, and HbA1c influenced the levels of serum tOC. Conclusion: Osteocalcin is involved in energy metabolism in pediatric subjects because it is consistently related to metabolic and anthropometric parameters. Systematic Review Registration: https://www.crd.york.ac.uk/prospero/, identifier: CRD42019138283.
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Physical mobility is essential to health, and patients often rate it as a high-priority clinical outcome. Digital mobility outcomes (DMOs), such as real-world gait speed or step count, show promise as clinical measures in many medical conditions. However, current research is nascent and fragmented by discipline. This scoping review maps existing evidence on the clinical utility of DMOs, identifying commonalities across traditional disciplinary divides. In November 2019, 11 databases were searched for records investigating the validity and responsiveness of 34 DMOs in four diverse medical conditions (Parkinson's disease, multiple sclerosis, chronic obstructive pulmonary disease, hip fracture). Searches yielded 19,672 unique records. After screening, 855 records representing 775 studies were included and charted in systematic maps. Studies frequently investigated gait speed (70.4% of studies), step length (30.7%), cadence (21.4%), and daily step count (20.7%). They studied differences between healthy and pathological gait (36.4%), associations between DMOs and clinical measures (48.8%) or outcomes (4.3%), and responsiveness to interventions (26.8%). Gait speed, step length, cadence, step time and step count exhibited consistent evidence of validity and responsiveness in multiple conditions, although the evidence was inconsistent or lacking for other DMOs. If DMOs are to be adopted as mainstream tools, further work is needed to establish their predictive validity, responsiveness, and ecological validity. Cross-disciplinary efforts to align methodology and validate DMOs may facilitate their adoption into clinical practice.
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INTRODUCTION/OBJECTIVES: Cutaneous involvement is often overlooked in rheumatoid arthritis (RA). We described cutaneous findings in outpatients attending a recent-onset cohort and identified factors associated with skin involvement and reduced (R) dermatological quality of life (DQoL). METHODS: Skin and rheumatological examinations were performed in 122 patients. DQoL was assessed through the Dermatology Life Quality Index (DLQI). Skin findings were classified as RA-specific and RA-nonspecific. Multiple regression analysis identified factors associated to skin involvement and RDQoL (DLQI score > 1). RESULTS: Patients were middle-aged females (91%), with a 1-year mean disease activity score in 28 joints as 2.0 (interquartile range: 1.5-2.6). There were 94 (77%) patients in whom at least one cutaneous finding was observed: 17 (13.1%) had RA-specific findings (all were rheumatoid nodules) and 91 (96.8%) had at least one RA-nonspecific finding, further classified into skin diseases (35.2%), hair diseases (20.9%), and skin-related signs (76.9%, among whom 94.3% had xerosis). Age (odds ratio [OR]: 1.054, 95% confidence interval [CI]: 1.015-1.094) and skin-health concerns (OR: 5.657, 95% CI: 1.771-18.070) were associated with cutaneous involvement, whereas increased age and DLQI score were associated with a higher number of skin findings/patient. There were 29 patients (24.2%) with RDQoL, which were associated with the Short Form-36 emotional component (OR: 0.955, 95% CI: 0.923-0.988) and the number of skin findings/patient (OR 2.873, 95% CI 1.723-4.791). Pruritus and hair diseases were the individual categories associated with RDQoL. CONCLUSIONS: Cutaneous manifestations are frequent in RA patients and have the potential to impact the emotional component of health-related quality of life. Key Points ⢠Up to 77% of the RA patients with substantial follow-up, from a recent-onset disease cohort, had cutaneous manifestations; these were primarily RA-nonspecific findings, whereas 13.1% had RA-specific findings. ⢠Skin-health concerns and age were associated with cutaneous involvement; meanwhile, increased age and Dermatology Life Quality Index (DLQI) score were associated with a higher number of cutaneous findings/patient. ⢠Reduced dermatological quality of life (RDQoL) was documented in one in four patients and was associated with the SF-36 emotional component and the number of cutaneous findings/patient.
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Artrite Reumatoide , Dermatopatias , Artrite Reumatoide/complicações , Artrite Reumatoide/epidemiologia , Estudos Transversais , Feminino , Humanos , Pessoa de Meia-Idade , Prurido , Qualidade de Vida , Dermatopatias/epidemiologiaRESUMO
OBJECTIVES: Cutaneous involvement is an extra-articular manifestation of rheumatoid arthritis (RA). This includes nail abnormalities, which are often overlooked. We described nail findings in RA patients currently attending an early arthritis cohort (n=145), and associated them with disease activity and/or damage, as well as patient-reported outcomes. METHODS: A standardised nail examination was performed in 122 patients (84.1% of the cohort), concomitant to the rheumatic assessment. Disability, quality of life and perceived nail-related health were also assessed. Nail findings and their location were recorded and classified according to standardised definitions. Logistic and linear regression models were used to investigate predictors of nail findings and to identify the impact of toenail findings on disability, which was evaluated with the HAQ. Patients consented to participate. RESULTS: Patients were primarily middle-aged females, with median follow-up of 9 years, and had disease under control. Most patients (62.3%) had at least one nail finding and these patients scored lower their nail-related health. The median (IQR) of findings/abnormalities per patient was 3 (2-5) and the number of nails affected per patient was 10 (2-12). Age (OR: 1.04, 95%CI: 1.007-1.074) and erosive disease (OR: 2.26, 95%CI: 1.1-5.1) were associated with nail findings. Toenail involvement was consistently associated with HAQ score out of normal range (OR=3.4, 95%CI=1.24-9.35, p=0.02). There was a linear association between the number of toenails affected and the HAQ score. CONCLUSIONS: Nail abnormalities are common and heterogeneous findings in RA patients; they are associated with erosive damage and impact disability.
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Artrite Reumatoide , Unhas Malformadas , Artrite Reumatoide/diagnóstico por imagem , Artrite Reumatoide/epidemiologia , Estudos Transversais , Avaliação da Deficiência , Feminino , Humanos , Pessoa de Meia-Idade , Unhas/diagnóstico por imagem , Unhas Malformadas/diagnóstico por imagem , Unhas Malformadas/epidemiologia , Unhas Malformadas/etiologia , Qualidade de Vida , Índice de Gravidade de DoençaRESUMO
BACKGROUND: The Mediterranean diet serves as a proxy of a high-quality diet. Although several factors are known to affect a child's ability to follow a high-quality diet, no prospective data are available on factors that influence adherence to a Mediterranean diet among children. Our objective was to investigate the association of Mediterranean diet adherence with eating behaviors, lifestyle habits, and maternal education in a prospective cohort of children. METHODS: The present prospective cohort analysis included 1639 children aged 8-10 years. The study was carried out during two academic years, 2012/2014, with an average follow-up of 15 months. Eating behaviors, physical activity, and adherence to Mediterranean diet were estimated by the Dutch Eating Behavior Questionnaire for Children, the Physical Activity Questionnaire for Children, and the KIDMED index, respectively. RESULTS: Multivariate linear regression analysis adjusted for sex, age, maternal education, baseline adherence to the Mediterranean diet, and intervention group revealed a significant (pâ¯<â¯0.01) inverse association of external eating and screen time with adherence to the Mediterranean diet at follow-up (mean of 15 months). The opposite association was found for meal frequency and physical activity (pâ¯<â¯0.02). A high level of maternal education increased the odds of a child's high adherence to the Mediterranean diet (ORâ¯=â¯1.56 CI 1.13; 2.14) compared to peers whose mothers had only a primary education. CONCLUSIONS: Screen time, physical activity, meal frequency, and external eating predict adherence to the Mediterranean diet independently of baseline diet quality. Maternal education level is an important prospective determinant for the adherence to the Mediterranean diet. TRIAL REGISTRATION NUMBER: ISRCTN68403446.
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Dieta Mediterrânea , Escolaridade , Comportamento Alimentar , Estilo de Vida , Mães , Criança , Exercício Físico , Feminino , Humanos , Masculino , Estudos Prospectivos , Tempo de Tela , Espanha , Inquéritos e QuestionáriosRESUMO
BACKGROUND: Plant-based diets have been linked to high diet quality and reduced risk of cardiovascular diseases. The health impact of plant-based diets might be partially explained by the concomitant intake of flavonoids. Estimation of flavonoids intake in adults has been important for the development of dietary recommendations and interventions for the prevention of weight gain and its consequences. However, estimation of flavonoids intake in children and adolescents is limited. METHODS: Average daily intake and sources of flavonoids were estimated for a representative national sample of 3,534 children and young people in Spain, aged 2-24 years. The data was collected between 1998 and 2000 by 24-h recalls. The Phenol-Explorer database and the USDA database on flavonoids content were used. Adherence to the Mediterranean diet was measured by the KIDMED index. RESULTS: The mean and median intakes of total flavonoids were 70.7 and 48.1 mg/day, respectively. The most abundant flavonoid class was flavan-3-ols (35.7%), with fruit being the top food source of flavonoids intake (42.8%). Total flavonoids intake was positively associated with the KIDMED index (p < 0.001). CONCLUSION: The results of this study provide primary information about flavonoids intake and main food sources in Spanish children, adolescents and young adults. Participants with high daily mean intake of flavonoids have higher adherence to the Mediterranean diet.
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Many chromosomal deletions encompassing the 2q23.1 region have been described ranging from small deletions of 38 kb up to >19 Mb. Most phenotypic features of the 2q23.1 deletion syndrome are due to a MBD5 gene loss independent of the size of the deletion. Here, we describe a male patient harboring a novel interstitial deletion encompassing the 2q22.3 q23.3 chromosomal region. Array-CGH revealed a 7.1 Mb deletion causing haploinsufficiency of several genes including MBD5, ACVR2, KIF5C, and EPC2. This patient presents with additional findings to those already described in individuals who have deletions of MBD5 including toes absence of halluces, pure red cell aplasia, and intestinal aganglionosis. Interestingly, in the deleted region there are previously identified regulatory sequences which are located upstream to ZEB2, which is associated with Hirschsprung disease (HSCR). Several genes have been associated with pure red cell aplasia, but to our knowledge, this is the first time that 2q deletion is associated with this phenotype. These additional findings should be added to the list of manifestations associated with 2q deletion, and provide support for the hypothesis that this individual has a true contiguous gene deletion syndrome.
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Osso e Ossos/anormalidades , Deleção Cromossômica , Cromossomos Humanos Par 2 , Aplasia Pura de Série Vermelha/genética , Hibridização Genômica Comparativa , Epilepsia/genética , Humanos , Recém-Nascido , MasculinoRESUMO
La información sobre biomarcadores óseos en adolescentes y adultas durante el periodo posparto es incierta, por lo que el objetivo de este artículo fue analizar el patrón de biomarcadores óseos en adolescentes y adultas a 15, 90, 180 y 365 días posparto (dpp) y su asociación con la densidad mineral ósea (DMO) y lactancia materna. Se realizó un estudio de cohorte en 32 madres adolescentes ≤17 años y 41 adultas de 18 a 29 años de edad en el primer año posparto. Se realizaron medidas antropométricas, DMO y biomarcadores óseos y así como datos del tipo y la duración de lactancia. Como resultados se encontró asociación entre la concentración basal de N-telopéptidos ≤24 μg/L y mayor aumento de DMO. Las adolescentes tuvieron mayor concentración de N-telopéptidos (p≤0.004) y menor concentración de osteocalcina (5±3 vs13±4, p <0.001) que las adultas. La lactancia no afectó el cambio de DMO (p>0.050), ni de biomarcadores óseos. La osteocalcina se asoció con el cambio en DMO (p<0.040). La prolactina fue mayor entre las que practicaron lactancia materna exclusiva (p<0.001). A menor edad menores concentraciones de osteocalcina (p<0.001) y mayores concentraciones de N-telopéptidos (p<0.001). Se concluyó que a menor concentración de N-telopéptidos y mayor de osteocalcina hubo un mayor aumento de DMO, lo cual implica menor aumento de ésta en el grupo de adolescentes. La lactancia no afectó la DMO.
The objective of this study was to describe the trend of bone biomarkers in adults and adolescents women at 15, 90, 180 and 365 postpartum days (ppd) and its relation with bone mineral density (BMD). It was a prospective cohort of 32 teenagers ≤17 and 41 women from 18 to 29 years old. We evaluated diet, anthropometry, BMD, bone biomarkers and hormonal profile. In all, the concentration of N-telopeptide was higher at 15 days postpartum decreasing during first year postpartum, but adolescents had the highest concentration. The lowest N-telopeptide concentration was associated with highest increasing of the BMD. Osteocalcin concentration was lower in adolescents than in adults women (5 ± 3 vs 13 ± 4 ng/mL, p<0.001) during first year postpartum. Exclusive breastfeeding did not affect the BMD (p>0.050) or bone biomarkers. Osteocalcin concentration was positively associated with bone BMD (p<0.040), breastfeeding did not affect osteocalcin concentrations. Prolactin was higher among women who breastfed exclusively (p<0.001). Age and breastfeeding inversely correlated with bone biomarkers (p<0.001) N-telopeptide and PTHi respectively. We concluded that a lower N-telopeptide concentration and a higher osteocalcin concentration were associated with a higher increasing of BMD, so then, adolescents showed the lowest recovery of the BMD. Breastfeeding does not affect the BMD.
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Adolescente , Adulto , Feminino , Humanos , Masculino , Adulto Jovem , Densidade Óssea/fisiologia , Colágeno Tipo I/sangue , Lactação/sangue , Osteocalcina/sangue , Peptídeos/sangue , Período Pós-Parto/sangue , Absorciometria de Fóton , Biomarcadores/sangue , Estudos de Coortes , Lactação/fisiologia , Período Pós-Parto/fisiologiaRESUMO
The objective of this study was to describe the trend of bone biomarkers in adults and adolescents women at 15, 90, 180 and 365 postpartum days (ppd) and its relation with bone mineral density (BMD). It was a prospective cohort of 32 teenager's ≤17 and 41 women from 18 to 29 years old. We evaluated diet, anthropometry, BMD, bone biomarkers and hormonal profile. In all, the concentration of N-telopeptide was higher at 15 days postpartum decreasing during first year postpartum, but adolescents had the highest concentration. The lowest N-telopeptide concentration was associated with highest increasing of the BMD. Osteocalcin concentration was lower in adolescents than in adults women (5 ± 3 vs 13 ± 4 ng/mL, p<0.001) during first year postpartum. Exclusive breastfeeding did not affect the BMD (p>0.050) or bone biomarkers. Osteocalcin concentration was positively associated with bone BMD (p<0.040), breastfeeding did not affect osteocalcin concentrations. Prolactin was higher among women who breastfed exclusively (p<0.001). Age and breastfeeding inversely correlated with bone biomarkers (p<0.001) N-telopeptide and PTHi respectively. We concluded that a lower N-telopeptide concentration and a higher osteocalcin concentration were associated with a higher increasing of BMD, so then, adolescents showed the lowest recovery of the BMD. Breastfeeding does not affect the BMD.
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Densidade Óssea/fisiologia , Colágeno Tipo I/sangue , Lactação/sangue , Osteocalcina/sangue , Peptídeos/sangue , Período Pós-Parto/sangue , Absorciometria de Fóton , Adolescente , Adulto , Biomarcadores/sangue , Estudos de Coortes , Feminino , Humanos , Lactação/fisiologia , Masculino , Período Pós-Parto/fisiologia , Adulto JovemRESUMO
El síndrome de Griscelli (SG) es una enfermedad autosómica recesiva, caracterizada, según las variantes clínicas, por albinismo parcial o cabello platinado, inmunodeficiencia celular, hipogammaglobulinemia, pancitopenia y severo deterioro neurológico. El diagnóstico se realiza de acuerdo a los hallazgos histopatológicos de la biopsia de piel, las manifestaciones clínicas descriptas y el análisis molecular de los genes RAB27A y MYO5A. Se describe un caso de SG, confirmado mediante estudio molecular, en una familia mexicana con antecedentes de consanguinidad tío paterno-sobrina y una hermana mayor con característiscas similares, fallecida a los 4 años. El paciente, al nacer, había tenido diagnóstico de albinismo. Se presentó a la consulta con historia de infecciones frecuentes y fiebres recurrentes sin foco y se encontró bicitopenia y síndrome mieloproliferativo. Ante la sospecha diagnóstica, se realizó una microscopía del cabello, en la que se observó distribución del pigmento en cúmulos y en los frotis hemáticos se determinó la ausencia de inclusiones intracitoplasmáticas. Se estableció el diagnóstico de SG tipo 2 y se obtuvo una muestra de ADN para el estudio molecular del gen RAB27A. El examen confirmó una mutación homocigota no comunicada previamente, por lo que se dedujo que su hermana había tenido la misma afección y que el padre era portador obligado...(AU)
Griscelli syndrome (GS) is an autosomal recessive disease characterized by partial albinism or platinum hair, varying cell immunodeficiency, hypogammaglobulinemia, pancytopenia and severe neurological impairment, depending on clinical variants. The diagnosis is made with histopathological findings in skin biopsy, the clinical manifestations described and molecular analysis of the genes RAB27A and MYO5A. We describe a case of GS, confirmed by molecular study, in a Mexican family with a history of paternal uncle-niece consanguinity and a sister with similar characteristics, deceased at 4 years old. At birth, the patient was diagnosed as albinism. He presented to us with a history of frequent infections and recurrent fevers of unknown origin and a bicytopenia and a myeloproliferative syndrome were found. With diagnostic suspicion, a mycroscopic study of the hair was done and the findings were consistent with pigment distribution in clusters and in hematological smears the absence of intracytoplasmic inclusions was demonstrated. Therefore the diagnosis of GS type 2 was established and a DNA sample was obtained for RAB27A gene molecular study. The exam confirmed a previously unreported homozygous mutation in the gene RAB27A, so it was established that his sister had the same condition and the father was a forced carrier...(AU)
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Humanos , Masculino , Pré-Escolar , Mutação , Albinismo , Transtornos da Pigmentação , Linfo-Histiocitose Hemofagocítica , Mutação em Linhagem GerminativaRESUMO
El síndrome de Griscelli (SG) es una enfermedad autosómica recesiva, caracterizada, según las variantes clínicas, por albinismo parcial o cabello platinado, inmunodeficiencia celular, hipogammaglobulinemia, pancitopenia y severo deterioro neurológico. El diagnóstico se realiza de acuerdo a los hallazgos histopatológicos de la biopsia de piel, las manifestaciones clínicas descriptas y el análisis molecular de los genes RAB27A y MYO5A. Se describe un caso de SG, confirmado mediante estudio molecular, en una familia mexicana con antecedentes de consanguinidad tío paterno-sobrina y una hermana mayor con característiscas similares, fallecida a los 4 años. El paciente, al nacer, había tenido diagnóstico de albinismo. Se presentó a la consulta con historia de infecciones frecuentes y fiebres recurrentes sin foco y se encontró bicitopenia y síndrome mieloproliferativo. Ante la sospecha diagnóstica, se realizó una microscopía del cabello, en la que se observó distribución del pigmento en cúmulos y en los frotis hemáticos se determinó la ausencia de inclusiones intracitoplasmáticas. Se estableció el diagnóstico de SG tipo 2 y se obtuvo una muestra de ADN para el estudio molecular del gen RAB27A. El examen confirmó una mutación homocigota no comunicada previamente, por lo que se dedujo que su hermana había tenido la misma afección y que el padre era portador obligado...
Griscelli syndrome (GS) is an autosomal recessive disease characterized by partial albinism or platinum hair, varying cell immunodeficiency, hypogammaglobulinemia, pancytopenia and severe neurological impairment, depending on clinical variants. The diagnosis is made with histopathological findings in skin biopsy, the clinical manifestations described and molecular analysis of the genes RAB27A and MYO5A. We describe a case of GS, confirmed by molecular study, in a Mexican family with a history of paternal uncle-niece consanguinity and a sister with similar characteristics, deceased at 4 years old. At birth, the patient was diagnosed as albinism. He presented to us with a history of frequent infections and recurrent fevers of unknown origin and a bicytopenia and a myeloproliferative syndrome were found. With diagnostic suspicion, a mycroscopic study of the hair was done and the findings were consistent with pigment distribution in clusters and in hematological smears the absence of intracytoplasmic inclusions was demonstrated. Therefore the diagnosis of GS type 2 was established and a DNA sample was obtained for RAB27A gene molecular study. The exam confirmed a previously unreported homozygous mutation in the gene RAB27A, so it was established that his sister had the same condition and the father was a forced carrier...
Assuntos
Humanos , Masculino , Pré-Escolar , Albinismo , Mutação , Transtornos da Pigmentação , Mutação em Linhagem Germinativa , Linfo-Histiocitose HemofagocíticaRESUMO
Introduction Acute porphyrias are rare genetic disorders of incomplete penetrance (10%). This means that only 10% of the individuals with the genotype known to cause the disease will show any signs or symptoms of such disease. They consist of a deficiency of any enzyme of the heme biosynthesis and are considered as exceptional inborn errors of metabolism with an autosomal dominant inheritance. The incidence is 1 in 100 000. The symptoms are variable and unspecific, consisting mainly of severe abdominal pain, tachycardia, and hypertension. Other frequent manifestations are psychiatric symptoms like depression, psychosis, and hallucinations. In addition to these unspecific symptoms, patients may also present peripheral neuropathy and loss of sensation, which can become permanent. In severe cases, liver damage and chronic renal disease can occur. The objective of this study is to highlight the importance of the difficult diagnosis of acute porphyria, the implications of a misdiagnosis, and the importance of adequate treatment. Case We present a 47 year-old male with a history of abdominal pain for seven years. The pain was diffuse, progressive, and incapacitating. He was diagnosed and treated for chronic gastritis and cholecystitis without improvement. An elective cholecystectomy was performed but he continued with intense abdominal pain. Three years later he developed hallucinations, paresthesias, muscular weakness, depression, and irritability. He was managed as a psychiatric patient with psychotic tendencies. After a complete and thorough history of all his symptoms throughout the years and a re-examination of the patient, acute porphyria was considered as a possible diagnosis. Specific laboratory studies were indicated revealing elevated levels of porphyrines, elevated levels of PBGD, PBG in urine within normal levels, elevated presence of coproporphyrines by chromatography, and a normal PBGD enzymatic activity. The diagnosis of acute porphyria was established. Appropriate treatment was initiated starting with adequate pain management. A high carbohydrate diet was also recommended with appropriate nutritional requirements and caloric intake. Another important aspect of the management was the elimination of risk factors, like alcohol, cigarette smoking, and certain specific medications. Follow-up showed significant improvement of his symptoms and less frequent acute attacks with identification and elimination of risk factors. He was able to return to a stable work schedule. The patient presents residual permanent renal damage. Adequate doctor-patient education was maintained. Discussion This case is an important example of a not-so-rare genetic disease that any physician should have in mind when confronted with a patient with unspecific paroxysmal clinical manifestations. The possibility of acute porphyria should always be excluded before establishing a diagnosis of a psychiatric illness. Prompt diagnosis and management are crucial to reduce the risk of recurrences and permanent damage. Patient education is a very important aspect of the management of the disease since there is no cure. There is a specific treatment for the management of acute attacks (Hemin) but, unfortunately, it is still unavailable in our country. This is a problem that turns the management and prevention of risk factors into the most important tools we have to improve our patients' quality of life.
Introducción Las porfirias agudas son un conjunto de enfermedades genéticas de penetrancia incompleta (10%). Es decir, sólo 10% de los individuos con el genotipo determinado que causa la enfermedad presentan algún signo o síntoma de ella. Las porfirias agudas son causadas por una deficiencia de alguna de las enzimas de la biosíntesis del heme. Son unos de los pocos errores innatos del metabolismo que presentan herencia autosómica dominante. La incidencia es de 1 en 100 000, y es más común en mujeres de entre 30-40 años. Los síntomas son variables e inespecíficos; los más comunes son: dolor abdominal difuso e incapacitante, taquicardia e hipertensión. También se acompaña de síntomas psiquiátricos como depresión, intento de suicidio, paranoia y alucinaciones. Otros síntomas relacionados son neuropatía periférica y pérdidas sensitivas, daño hepático e insuficiencia renal crónica. El objetivo de este estudio es establecer la importancia de realizar un diagnóstico oportuno de porfiria aguda, ya que un diagnóstico erróneo puede generar tratamientos y gastos innecesarios al paciente. El diagnóstico de porfiria permite llevar a cabo un manejo y tratamiento adecuados que favorecen un buen pronóstico. Caso Se trata de un paciente masculino de 47 años de edad, sin antecedentes familiares relacionados, que presenta dolor abdominal intenso, difuso e incapacitante con siete años de evolución. Fue tratado como gastritis aguda y colecistitis. Se realizó colecistectomía sin lograr mejoría de los síntomas. Tres años después, se agregaron a los síntomas originales los siguientes: alucinaciones auditivas, parestesias, debilidad muscular, depresión e irritabilidad, por lo que se catalogó como paciente con trastorno psiquiátrico con tendencia psicótica. Se realizó historia clínica de todos los síntomas y una exploración física completa, por lo que se sospechó porfiria aguda. Se realizaron estudios de laboratorio específicos con los que se confirmó el diagnóstico de porfiria aguda por la presencia de niveles elevados de porfirinas en orina, niveles elevados de PBGD, niveles normales de PBG en orina, niveles significativamente elevados de coproporfirinas por cromatografía y actividad enzimática de PBGD en rangos normales. Se inició un tratamiento para el manejo adecuado del dolor. También, una dieta alta en carbohidratos, con aporte calórico adecuado. Se recomendó la eliminación de factores de riesgo como alcohol, cigarro y medicamentos específicos. Dos meses después se observó una mejoría significativa de los síntomas, control de crisis e identificación y eliminación de factores precipitantes. Los síntomas psiquiátricos desaparecieron y el paciente pudo reestablecer sus actividades laborales y sociales. El paciente presenta hasta el momento datos de insuficiencia renal crónica. Se continúa el seguimiento del paciente. Discusión El caso presentado representa un ejemplo de una enfermedad genética que todo médico debe tener en mente cuando se presenta un paciente con síntomas inespecíficos. El diagnóstico de porfiria aguda es un diagnóstico de exclusión, pero sigue siendo importante en el análisis del diagnóstico diferencial. Es de gran importancia descartar o confirmar un caso de porfiria aguda antes de establecer el diagnóstico de un trastorno psiquiátrico. Establecer un diagnóstico temprano y un tratamiento específico mejora el pronóstico y limita el daño, particularmente neurológico y hepático. La educación del paciente es de extrema importancia, ya que no existe cura para la porfiria aguda. Una prevención que evite los factores precipitantes conocidos es uno de los tratamientos principales de esta enfermedad, ya que el medicamento específico para el control de la crisis aguda (Hematina) no se distribuye en nuestro país. Aunado a un subdiagnóstico de la enfermedad, lo anterior vuelve aún más difícil el manejo de los pacientes.
RESUMO
Introducción. Objetivo: evaluar el cumplimiento de la "Guía de salud para personas con síndrome de Down" de la Asociación Americana de Pediatría de 2001 en pacientes del Departamento de Genética del Hospital Universitario "Dr. José Eleuterio González . Métodos. Estudio retrospectivo, descriptivo, observacional y transversal, en el cual se revisaron los expedientes de pacientes con síndrome de Down que acudieron a consulta al Departamento de Genética entre abril de 2004 y abril de 2006. Resultados. Se identificaron 38 casos. El límite de edad materna fue de 17-43 años. En 74% de los pacientes se realizó cariotipo y sólo 61% recibieron asesoría genética. Se identificó cardiopatía congénita por ecocardiograma en 26%, pero en 56% no se realizaron estudios a pesar de contar con datos clínicos sugestivos. El número máximo de consultas fue de 5; sin embargo, 44% de los pacientes no tuvo seguimiento. Conclusiones. Se identificó una falla importante en la adherencia al seguimiento y a la realización de estudios encaminados a descartar las complicaciones asociadas al síndrome.
Introduction. Objective: To evaluate the application of the American Academy of Pediatrics' "Guidelines for health supervision for children with Down syndrome" in the Department of Genetics at the Hospital Universitario "Dr. José Eleuterio González". Methods. We analyzed clinical files from all Down's syndrome patients who attended our Department of Genetics from April 2004 to April 2006. Results. Thirty-eight cases were identified. The rank of mothers' age at date of infant birth was 17-43 years old; 74% of the patients had a karyotype performed, but genetic counseling was given only to 61% of families. An echocardiogram was performed; congenital heart disease was detected in 26%, but 56% did not attend the cardiologist consultation even when some of them had clinical findings suggesting heart disease. At the end of the study, the highest number of consultations was 5; however, 44% of the patients had no follow-up. Conclusions. We found a significant lack of commitment to follow-up patients by care givers, and a delay to accomplish clinical studies to avoid the well-known complications associated to this syndrome.
