12 results on '"Baranov, Esther"'
Search Results
2. Histologic characterization of paediatric mesenchymal neoplasms treated with kinase‐targeted therapy.
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Baranov, Esther, Winsnes, Katrina, O'Brien, Matthew, Voss, Stephan D, Church, Alanna J, Janeway, Katherine A, DuBois, Steven G, Davis, Jessica L, and Al‐Ibraheemi, Alyaa
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TUMORS , *ANAPLASTIC lymphoma kinase , *CELL tumors , *PROTEIN-tyrosine kinases , *PEDIATRICS , *REGULATORY approval , *FIBROSARCOMA - Abstract
Aims: Recurrent alterations involving receptor tyrosine or cytoplasmic kinase genes have been described in soft‐tissue neoplasms such as infantile fibrosarcoma (IFS) and inflammatory myofibroblastic tumour (IMT). Recent trials and regulatory approvals for targeted inhibitors against the kinase domains of these oncoproteins have allowed for increased use of targeted therapies. We aimed to characterize the histologic features of paediatric mesenchymal neoplasms with kinase alterations treated with targeted inhibitors. Methods and results: Eight patients with tyrosine kinase‐altered mesenchymal neoplasms with pre‐ and posttreatment samples were identified. Tumours occurred in five females and three males with a median age at presentation of 6.5 years. Tumour sites were bone/somatic soft‐tissue (n = 5) and viscera (n = 3). Pretreatment diagnoses were: IMT (n = 3), epithelioid inflammatory myofibroblastic sarcoma (n = 1), and descriptive diagnoses (n = 4) such as "kinase‐driven spindle cell tumor." Fusions identified were ETV6::NTRK3 (n = 2), TPM3::NTRK1, SEPT7::BRAF, TFG::ROS1, KLC1::ALK, RANBP2::ALK, and MAP4::RAF1. Patients were treated with larotrectinib (n = 3), ALK or ALK/ROS1 inhibitors (n = 3), and MEK inhibitors (n = 2). Posttreatment tumours exhibited a striking decrease in cellularity (7/8) and the presence of collagenous stroma (7/8) with extensive glassy hyalinization (5/8). In two cases, abundant coarse or psammomatous calcifications were seen and in one case prominent perivascular hyalinization was noted. Residual viable tumour was seen in 3/8 cases (<5% in one case, and >75% in 2/8 cases). Conclusion: Mesenchymal neoplasms with tyrosine kinase alterations treated with targeted inhibitors show a pathologic response, which includes decreased cellularity and stromal hyalinization. The presence of these features may be helpful in assessing tumour response after targeted therapy. [ABSTRACT FROM AUTHOR]
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- 2022
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3. Persistent decrease in multiple components of the perineuronal net following status epilepticus.
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McRae, Paulette A., Baranov, Esther, Rogers, Stephanie L., and Porter, Brenda E.
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STATUS epilepticus , *TEMPORAL lobe epilepsy , *AGGRECAN , *PROTEOGLYCANS , *HIPPOCAMPUS (Brain) , *LABORATORY rodents , *EXTRACELLULAR matrix - Abstract
In the rodent model of temporal lobe epilepsy, there is extensive synaptic reorganization within the hippocampus following a single prolonged seizure event, after which animals eventually develop epilepsy. The perineuronal net (PN), a component of the neural extracellular matrix (ECM), primarily surrounds inhibitory interneurons and, under normal conditions, restricts synaptic reorganization. The objective of the current study was to explore the effects of status epilepticus (SE) on PNs in the adult hippocampus. The aggrecan component of the PN was studied, acutely (48 h post-SE), sub-acutely (1 week post-SE) and during the chronic period (2 months post-SE). Aggrecan expressing PNs decreased by 1 week, likely contributing to a permissive environment for neuronal reorganization, and remained attenuated at 2 months. The SE-exposed hippocampus showed many PNs with poor structural integrity, a condition rarely seen in controls. Additionally, the decrease in the aggrecan component of the PN was preceded by a decrease in hyaluronan and proteoglycan link protein 1 (HAPLN1) and hyaluronan synthase 3 (HAS3), which are components of the PN known to stabilize the connection between aggrecan and hyaluronan, a major constituent of the ECM. These results were replicated in vitro with the addition of excess KCl to hippocampal cultures. Enhanced neuronal activity caused a decrease in aggrecan, HAPLN1 and HAS3 around hippocampal cells in vivo and in vitro, leaving inhibitory interneurons susceptible to increased synaptic reorganization. These studies are the foundation for future experiments to explore how loss of the PN following SE contributes to the development of epilepsy. [ABSTRACT FROM AUTHOR]
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- 2012
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4. Aggrecan expression, a component of the inhibitory interneuron perineuronal net, is altered following an early-life seizure
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McRae, Paulette A., Baranov, Esther, Sarode, Shilpa, Brooks-Kayal, Amy R., and Porter, Brenda E.
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SPASMS , *PROTEOGLYCANS , *EXTRACELLULAR matrix , *HIPPOCAMPUS (Brain) , *INTERNEURONS , *NEURAL physiology , *GENE expression - Abstract
Abstract: The perineuronal net (PN), a component of the neural extracellular matrix (ECM), is a dynamic structure whose expression decreases following diminished physiological activity. Here, we analyzed the effects of increased neuronal activity on the development of aggrecan, a component of the PN, in the hippocampus. We show aggrecan expression to be prominent around parvalbumin (PV) interneurons in the postnatal hippocampus. Moreover, after seizure induction in early life there was a significant increase in aggrecan expression in a region specific manner during the course of development. We conclude that increased neuronal activity leads to accelerated expression of PNs in the hippocampus that attenuates in the adult hippocampus. This study shows the dynamic nature of the PN component of the ECM and the role neuronal activity has in molding the extracellular milieu of inhibitory interneurons. [Copyright &y& Elsevier]
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- 2010
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5. A metagenomic analysis of the virome of inverted papilloma and squamous cell carcinoma.
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Tong, Charles C. L., Lin, Xiang, Seckar, Tyler, Koptyra, Mateusz, Kohanski, Michael A., Cohen, Noam A., Kennedy, David W., Adappa, Nithin D., Papagiannopoulos, Peter, Kuan, Edward C., Baranov, Esther, Jalaly, Jalal B., Feldman, Michael D., Storm, Phillip B., Resnick, Adam C., Palmer, James N., Wei, Zhi, and Robertson, Erle S.
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PAPILLOMA , *SQUAMOUS cell carcinoma , *HUMAN papillomavirus , *METAGENOMICS , *VIRAL genomes , *CARCINOMA in situ - Abstract
Introduction: Inverted papilloma (IP) is a sinonasal tumor with a well‐known potential for malignant transformation. The role of human papillomavirus (HPV) in its pathogenesis has been controversial. The purpose of this study was to determine the virome associated with IP, with progression to carcinoma in situ (CIS), and invasive carcinoma. Methods: To determine the HPV‐specific types, a metagenomics assay that contains 62,886 probes targeting viral genomes in a microarray format was used. The platform screens DNA and RNA from fixed tissues from eight controls, 16 IP without dysplasia, five IP with CIS, and 13 IP‐associated squamous cell carcinoma (IPSCC). Paired with next‐generation sequencing, 48 types of HPV with 857 region‐specific probes were interrogated against the tumors. Results: The prevalence of HPV‐16 was 14%, 42%, 70%, and 73% in control tissue, IP without dysplasia, IP with CIS, and IPSCC, respectively. The prevalence of HPV‐18 had a similar progressive increase in prevalence, with 14%, 27%, 67%, and 74%, respectively. The assay allowed region‐specific analysis, which identified the only oncogenic HPV‐18 E6 to be statistically significant when compared with control tissue. The prevalence of HPV‐18 E6 was 0% in control tissue, 25% in IP without dysplasia, 60% in IP with CIS, and 77% in IPSCC. Conclusions: There are over 200 HPV types that infect human epithelial cells, of which only a few are known to be high‐risk. Our study demonstrated a trend of increasing prevalence of HPV‐18 E6 that correlated with histologic severity, which is novel and supports a potential role for HPV in the pathogenesis of IP. [ABSTRACT FROM AUTHOR]
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- 2023
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6. Perineuronal net degradation in epilepsy.
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Rankin‐Gee, Elyse K., McRae, Paulette A., Baranov, Esther, Rogers, Stephanie, Wandrey, Luke, and Porter, Brenda E.
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PARVALBUMINS , *IMMUNOHISTOCHEMISTRY , *MATRIX metalloproteinases , *PILOCARPINE , *PROTEOLYSIS ,EPILEPSY research - Abstract
Objective We previously reported loss of perineuronal net ( PN) immunohistochemical staining around parvalbumin-positive interneurons in the hippocampus of rats after an episode of status epilepticus ( SE). We hypothesized that the loss of the PN could alter seizure susceptibility and that matrix metalloproteinases ( MMPs) were candidates for degradation of the PN following SE. Methods The pilocarpine chemoconvulsant rodent epilepsy model was used to characterize the degradation of the aggrecan component of the PN in the hippocampus following SE. Chondroitinase ABC (Ch ABC) was used to degrade the PN in mice. Onset, number, and duration of pentylenetetrazole ( PTZ)-induced seizures were assessed. Results The loss of the PN in the hippocampus following SE is at least partially related to degradation of the aggrecan PN component by MMP activity. Forty-eight hours after SE, a neoepitope created by MMP cleavage of aggrecan was present and concentrated around parvalbumin-positive interneurons. The increase in aggrecan cleavage products was found at 48 h, 1 week, and 2 months after SE, with different fragments predominating over time. We demonstrate ongoing aggrecan proteolysis and fragment accumulation in the hippocampus of adult control rats, as well as in SE-treated animals. Degradation of the PN alters the seizure response to PTZ. ChABC treatment caused an increase in myoclonic seizures following PTZ administration, a delayed onset of Racine stage 4/5 seizure, and a decreased duration of Racine stage 4/5 seizure. Significance Status epilepticus increases MMP proteolysis of aggrecan, pointing to MMP activity as one mechanism of PN degradation post- SE. There is accumulation of aggrecan fragments in adult rat hippocampus of both control and SE-exposed animals. Loss of the PN was associated with increased numbers of myoclonic seizures; it also, delayed and shortened the duration of Racine stage 4/5 seizures, suggesting a complex relationship between the PN and seizure susceptibility. [ABSTRACT FROM AUTHOR]
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- 2015
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7. Targeted gene expression profiling of inverted papilloma and squamous cell carcinoma.
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Tong, Charles C. L., Koptyra, Mateusz, Raman, Pichai, Rathi, Komal S., Choudhari, Namrata, Lin, Xiang, Seckar, Tyler, Wei, Zhi, Kohanski, Michael A., O'Malley, Bert W., Cohen, Noam A., Kennedy, David W., Adappa, Nithin D., Robertson, Erle S., Baranov, Esther, Kuan, Edward C., Papagiannopoulos, Peter, Jalaly, Jalal B., Feldman, Michael D., and Storm, Phillip B.
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GENE expression profiling , *SQUAMOUS cell carcinoma , *EPITHELIAL-mesenchymal transition , *PAPILLOMA , *NUCLEOTIDE sequencing - Abstract
Background: Inverted papilloma (IP) is a sinonasal tumor with a well‐known potential for malignant transformation. The purpose of this study was to identify the genes and pathways associated with IP, with progression to carcinoma‐in‐situ and invasive carcinoma. Methods: To determine genes and molecular pathways that may indicate progression and correlate with histologic changes, we analyzed six IP without dysplasia, five IP with carcinoma‐in‐situ, and 13 squamous cell carcinoma ex‐IP by targeted sequencing. The HTG EdgeSeq Oncology Biomarker Panel coupled with next‐generation sequencing was used to evaluate 2560 transcripts associated with solid tumors. Results: Progressive upregulation of 11 genes were observed (CALD1, COL1A1, COL3A1, COL4A2, COL5A2, FN1, ITGA5, LGALS1, MMP11, SERPINH1, SPARC) in the order of invasive carcinoma > carcinoma‐in‐situ > IP without dysplasia. When compared with IP without dysplasia, more genes are differentially expressed in invasive carcinoma than carcinoma‐in‐situ samples (341 downregulated/333 upregulated vs. 195 downregulated/156 upregulated). Gene set enrichment analysis determined three gene sets in common between the cohorts (epithelial mesenchymal transition, extracellular matrix organization, and coagulation). Conclusions: Progressive upregulation of genes specific to IP malignant degeneration has significant clinical implications. This panel of 11 genes will improve concordance of histologic classification, which can directly impact treatment and patient outcomes. Additionally, future studies on larger tumor sets may observe upregulation in the gene panel that preceded histologic changes, which may be useful for further risk stratification. [ABSTRACT FROM AUTHOR]
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- 2022
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8. 75. Clinical implementation of a precision medicine consultation service.
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Finer, Abigail, Pannone, Andrea, Bard, Adam, Green, Ursula, Baranov, Esther, Ritterhouse, Lauren, Dias-Santagata, Dora, and Lennerz, Jochen
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INDIVIDUALIZED medicine , *SYSTEM integration , *MANAGEMENT information systems , *INFORMATION resources management , *ELECTRONIC health records , *MEDICAL technologists - Abstract
To realize precision medicine, clinicians need to apply a growing number of diagnostic tests. Each test result relies on specific domain expertise; however, integration across a variety of diagnostics poses unique challenges-including financial sustainability of the consultation service. Recent 2022 billing code updates emphasize the value of consultations. Here, we present the design and implementation of a clinical pathology consultation workflow. The core design team consisted of 3 board-certified molecular-genetic pathologists, 1 board-certified genetic counselor, and 1 high-complexity medical technologist. Additional team members included billing operations, electronic medical record (EMR) support staff, compliance, departmental, hospital, and network leadership. The team focused on a modular, EMR-based design with laboratory information management system integration, and compliant documentation and billing practices. The 7-month design process consisted of weekly 30-90 min meetings of the core team supplemented by various meetings with additional team members (estimated total effort ∼170h or ∼10% of a full-time position). The workflow consisted of 7 modules: (1) physician order, (2) triaging module, (3) e-reply no bill, (4) written documentation (limited, without billing), (5) written EMR documentation (comprehensive, with effort-based billing), (6) denial/appeal module, (7) direct patient question module. Since go-live in early 2022, we managed 22 consultations (n=6 comprehensive; n=16 billing-related questions) from 3 network sites. Realizing a precision medicine consultation workflow required significant effort from an interdisciplinary team. The workflow accounted for various administrative and compliance-related aspects and future work will focus on reimbursement, utilization, provider adoption, and optimization of workflows. [ABSTRACT FROM AUTHOR]
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- 2022
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9. Risk Factors for Cerebral Palsy in Children in Botswana.
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Monokwane, Baphaleng, Johnson, Allison, Gambrah-Sampaney, Claudia, Khurana, Esha, Baier, James, Baranov, Esther, Westmoreland, Kate D., Mazhani, Loeto, Steenhoff, Andrew P., and Bearden, David R.
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CEREBRAL palsy , *CHILDREN with cerebral palsy , *DISEASE prevalence , *RESOURCE allocation , *DISEASE risk factors , *HIV infections , *LOGISTIC regression analysis , *DISEASE incidence , *RETROSPECTIVE studies , *CASE-control method , *ODDS ratio , *DIAGNOSIS - Abstract
Background: Although cerebral palsy is reported to have a higher prevalence in low-resource settings, there are few studies describing risk factors for cerebral palsy in these settings. A better understanding of the unique risk factors affecting children with cerebral palsy in low-resource settings could optimize both resource allocation and preventative strategies.Methods: A case-control study comparing children with cerebral palsy at ages two to 18 years with age-matched healthy control subjects was conducted between 2013 and 2014 at a referral center in Gaborone, Botswana. Study participants were enrolled from inpatient and outpatient settings, and data were collected through caregiver interviews, review of medical records, and physical examination of subjects. Risk factors were evaluated using conditional logistic regression models.Results: We studied 56 subjects with cerebral palsy and 56 age-matched control subjects. Significant risk factors for cerebral palsy included a history of serious neonatal infection (odds ratio 15.0, P = 0.009), complications during delivery (odds ratio 13.5, P < 0.001), and maternal human immunodeficiency virus (HIV) infection (odds ratio 3.5, P = 0.03). Maternal HIV infection remained a significant risk factor after adjusting for potential confounders and covariates (adjusted odds ratio 13.2, P = 0.05).Conclusions: Major risk factors for cerebral palsy in Botswana differ from those described in high-resource settings. Modifiable risk factors such as maternal HIV infection should be targeted as a potential strategy to reduce the incidence of cerebral palsy in Botswana. Further studies are necessary to determine optimal preventative and treatment strategies in this population. [ABSTRACT FROM AUTHOR]- Published
- 2017
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10. Risk Factors for Malnutrition Among Children With Cerebral Palsy in Botswana.
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Johnson, Allison, Gambrah-Sampaney, Claudia, Khurana, Esha, Baier, James, Baranov, Esther, Monokwane, Baphaleng, and Bearden, David R.
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MALNUTRITION diagnosis , *CHILDREN with cerebral palsy , *MEDICAL screening , *TERTIARY care , *MALNUTRITION , *CEREBRAL palsy , *DEMOGRAPHY , *SOCIOECONOMIC factors , *RETROSPECTIVE studies , *CASE-control method , *RECEIVER operating characteristic curves , *ODDS ratio - Abstract
Background: Children with cerebral palsy in low-resource settings are at high risk of malnutrition, which further increases their risk of poor health outcomes. However, there are few available data on specific risk factors for malnutrition among children with cerebral palsy in the developing world.Methods: We performed a case-control study among children with cerebral palsy receiving care at a tertiary care hospital in Gaborone, Botswana. Children with cerebral palsy and malnutrition were identified according to World Health Organization growth curves and compared with subjects with cerebral palsy without malnutrition. Risk factors for malnutrition were identified using multivariable logistic regression models. These risk factors were then used to generate a Malnutrition Risk Score, and Receiver Operating Characteristic curves were used to identify optimal cutoffs to identify subjects at high risk of malnutrition.Results: We identified 61 children with cerebral palsy, 26 of whom (43%) met criteria for malnutrition. Nonambulatory status (odds ratio 13.8, 95% confidence interval [CI] 3.8-50.1, P < 0.001) and a composite measure of socioeconomic status (odds ratio 1.6, 95% CI 1.0-2.5, P = 0.03) were the strongest risk factors for malnutrition. A Malnutrition Risk Score was constructed based on these risk factors, and receiver operating characteristic curve analysis demonstrated excellent performance characteristics of this score (area under the curve 0.92, 95% CI 0.89-0.94).Conclusions: Malnutrition is common among children with cerebral palsy in Botswana, and a simple risk score may help identify children with the highest risk. Further studies are needed to validate this screening tool and to determine optimal nutritional interventions in this population. [ABSTRACT FROM AUTHOR]- Published
- 2017
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11. Increased metalloproteinase activity in the hippocampus following status epilepticus.
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Dubey, Deepti, McRae, Paulette A., Rankin-Gee, Elyse K., Baranov, Esther, Wandrey, Luke, Rogers, Stephanie, and Porter, Brenda E.
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MATRIX metalloproteinases , *STATUS epilepticus , *HIPPOCAMPUS physiology , *NEUROPLASTICITY , *PERINEURONAL nets - Abstract
Increased neuronal plasticity and neuronal cell loss has been implicated in the development of epilepsy following injury. Parvalbumin fast spiking inhibitory interneurons have a robust extracellular matrix coating their cell bodies and the proximal dendrites called the perineuronal net (PNN). The role of the PNN is not clear but it has been implicated in closing of the critical period, altering seizure thresholds and providing neuronal protection from oxidative stress. The PNN is susceptible to degradation following a prolonged seizure and there is an increase in proteolytic-fragments of the PNN enriched proteoglycan aggrecan (Dzwonek et al., 2004). Here we demonstrate an increase in matrix metalloproteinase (MMP) activity in the hippocampus following status epilepticus (SE). We further assessed MMP3 and 13, two of 24 identified MMPs, both MMP3 and 13 mRNA increase in the hippocampus after SE and MMP13 activity increases by functional assay as well as it co-localizes with PNN in rat brain. In contrast, two of the brain expressed ADAMTS (A Disintegrin And Metalloproteinase with ThromboSpondin motifs) also implicated in aggrecan degradation, did not consistently increase following SE though ADAMTS4 is highly expressed in glia and ADAMTS5 in neuronal cell bodies and their processes. The increase in MMP activity following SE suggests that in the future studies, MMP inhibitors are candidates for blocking PNN degradation and assessing the role of the PNN loss in epileptogenesis and cellular function. [ABSTRACT FROM AUTHOR]
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- 2017
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12. Pediatric Cerebral Palsy in Botswana: Etiology, Outcomes, and Comorbidities.
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Bearden, David R., Monokwane, Baphaleng, Khurana, Esha, Baier, James, Baranov, Esther, Westmoreland, Kate, Mazhani, Loeto, and Steenhoff, Andrew P.
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CEREBRAL palsy treatment , *JUVENILE diseases , *MOVEMENT disorders , *ETIOLOGY of diseases , *PERIODIC health examinations , *CROSS-sectional method , *CEREBRAL palsy , *LONGITUDINAL method , *RESEARCH funding , *COMORBIDITY , *SOCIOECONOMIC factors - Abstract
Background: Cerebral palsy is the most common cause of motor dysfunction in children worldwide and is often accompanied by multiple comorbidities. Although cerebral palsy has been studied extensively in high-resource settings, there are few published studies on cerebral palsy etiology, outcomes and comorbidities in low-resource settings.Methods: Children with cerebral palsy were prospectively enrolled from inpatient and outpatient settings at a referral center in Gaborone, Botswana, in a cross-sectional study conducted from 2013 to 2014. Cerebral palsy etiology, outcomes, and comorbidities were determined through caregiver interviews, review of medical records, and direct physical examination.Results: Sixty-eight children with cerebral palsy were enrolled. Subjects were 41% male, with a median age of 4 years (interquartile range = 2 to 7). The most common etiologies for cerebral palsy in our cohort were intrapartum hypoxic events (18%), postnatal infections (15%), prematurity (15%), focal ischemic strokes (10%), and prenatal infections (10%). Severe motor impairment was common, with the most severe category present in 41%. The predominant comorbidities were cognitive impairment (84%), epilepsy (77%), and visual impairment (46%).Conclusions: Cerebral palsy in Botswana has different etiologies and is associated with poorer outcomes and higher prevalence of comorbidities than what has been reported in high-resource settings. Further studies are necessary to determine optimal preventative and treatment strategies in this population. [ABSTRACT FROM AUTHOR]- Published
- 2016
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