Your search keyword '"J, El Dahr"' showing total 17 results

1. Seven novel mutations in the adenosine deaminase (ADA) gene in patients with severe and delayed onset combined immunodeficiency: G74C, V129M, G140E, R149W, Q199P, 462delG, and E337del. Mutations in brief no. 142. Online

Author

F X, Arrendondo-Vega, I, Santisteban, L D, Notarangelo, J, El Dahr, R, Buckley, C, Roifman, M E, Conley, and M S, Hershfield

Subjects

Adult, Adolescent, Proline, Adenosine Deaminase, Glutamine, Glycine, Tryptophan, Glutamic Acid, Valine, Arginine, Methionine, Mutation, Humans, Severe Combined Immunodeficiency, Cysteine, Age of Onset, Sequence Deletion

Abstract

The degree of immunodeficiency associated with deficiency of adenosine deaminase (ADA) is variable. Most patients are infants with severe combined immunodeficiency (SCID), but in about 20 percent immune dysfunction becomes manifest later in childhood ("delayed-onset"); several patients with "late" or "adult" onset of immune dysfunction have been diagnosed at 15-39 years. Over 40 ADA gene mutations have thus far been identified. To better define the genotype-phenotype relationship, we report 7 novel ADA mutations, including 5 missense mutations (G74C, V129M, G140E, R149W, Q199P) and two short deletions (462delG, E337del). These were identified among 7 patients (3 with SCID and 4 with delayed-onset). A homozygote for 462delG had SCID, whereas patients homozygous or heterozyous for V129M had delayed-onset. Two other delayed-onset patients, one heterozygous for G74C and the other for Q199P, each had a second allele carrying the previously reported "severe" mutation G216R. These findings are consistent with previous observations suggesting that, in general, SCID occurs when both alleles eliminate ADA function, and a milder phenotype when at least one allele can supply a low level of function.

Published

1999

2. Failure to thrive, diarrhea, cough, and oral candidiasis in a three-month-old boy

Author

D W, Walcott, T, Linehan, B C, Hilman, M S, Hershfield, and J, el Dahr

Subjects

Diarrhea, Male, Acquired Immunodeficiency Syndrome, Cystic Fibrosis, Adenosine Deaminase, Infant, Failure to Thrive, Wiskott-Aldrich Syndrome, Diagnosis, Differential, Cough, Candidiasis, Oral, Animals, Humans, Severe Combined Immunodeficiency, Rabbits, Follow-Up Studies

Published

1994

3. Seven novel mutations in the adenosine deaminase (ADA) gene in patients with severe and delayed onset combined immunodeficiency: G74C, V129M, G140E, R149W, Q199P, 462delG, and E337del

Author

J. El Dahr, Lucia Dora Notarangelo, Mary Ellen Conley, Rebecca H. Buckley, Francisco X. Arredondo-Vega, Chaim M. Roifman, Ines Santisteban, and Hershfield

Subjects

Severe combined immunodeficiency, Mutation, Biology, Gene mutation, medicine.disease, medicine.disease_cause, Adenosine deaminase, Immunology, Genetics, medicine, biology.protein, Missense mutation, Allele, Gene, Genetics (clinical), Immunodeficiency

Abstract

The degree of immunodeficiency associated with deficiency of adenosine deaminase (ADA) is variable. Most patients are infants with severe combined immunodeficiency (SCID), but in about 20 percent immune dysfunction becomes manifest later in childhood ("delayed-onset"); several patients with "late" or "adult" onset of immune dysfunction have been diagnosed at 15–39 years. Over 40 ADA gene mutations have thus far been identified. To better define the genotype-phenotype relationship, we report 7 novel ADA mutations, including 5 missense mutations (G74C, V129M, G140E, R149W, Q199P) and two short deletions (462delG, E337del). These were identifed among 7 patients (3 with SCID and 4 with delayed-onset). A homozygote for 462delG had SCID, whereas patients homozygous or heterozygous for V129M had delayed-onset. Two other delayed-onset patients, one heterozygous for G74C and the other for Q199P, each had a second allele carrying the previously reported "severe" mutation G216R. These findings are consistent with previous observations suggesting that, in general, SCID occurs when both alleles eliminate ADA function, and a milder phenotype when at least one allele can supply a low level of function. Hum Mutat 11:482, 1998. © 1998 Wiley-Liss, Inc.

Published

1998

4. Seven novel mutations in the adenosine deaminase (ADA) gene in patients with severe and delayed onset combined immunodeficiency: G74C, V129M, G140E, R149W, Q199P, 462delG, and E337del

Author

F. X. Arredondo‐Vega, I. Santisteban, L. D. Notarangelo, J. El Dahr, R. Buckley, C. Roifman, M. E. Conley, and M.S. Hershfield

Subjects

Genetics, Genetics (clinical)

Published

1998

5. Evidence of neuroinflammation and immunotherapy responsiveness in individuals with down syndrome regression disorder.

Author

Santoro JD, Partridge R, Tanna R, Pagarkar D, Khoshnood M, Rehmani M, Kammeyer RM, Gombolay GY, Fisher K, Conravey A, El-Dahr J, Christy AL, Patel L, Manning MA, Van Mater H, Rafii MS, and Quinn EA

Subjects

Activities of Daily Living, Case-Control Studies, Humans, Immunotherapy methods, Neuroinflammatory Diseases, Retrospective Studies, Down Syndrome complications, Down Syndrome therapy

Abstract

Background: Down syndrome regression disorder is a symptom cluster consisting of neuropsychiatric regression without cause. This study evaluated the incidence of neurodiagnostic abnormalities in individuals with Down syndrome regression disorder and determined if abnormalities are indicative of responses to therapeutic intervention., Methods: A retrospective, multi-center, case-control study was performed. Patients were required to have subacute onset and the presence of four of five symptom groups present (cognitive decline, expressive language, sleep derangement, loss of ability to perform activities of daily living, and/or a new movement disorder) and no other explanation for symptoms., Results: Individuals with Down syndrome regression disorder were comparable to a cohort of individuals with only Down syndrome although had higher rates of autoimmune disease (p = 0.02, 95%CI 1.04-1.75). Neurodiagnostic abnormalities were found on EEG (n = 19, 26%), neuroimaging (n = 16, 22%), and CSF (n = 9, 17%). Pleocytosis was appreciated in five cases, elevated total protein in nine, elevated IgG index in seven, and oligoclonal bands in two. Testing within 2 years of symptom onset was more likely to have neurodiagnostic abnormalities (p = 0.01, 95%CI 1.64-37.06). In individuals with neurodiagnostic abnormalities, immunotherapy was nearly four times more likely to have a therapeutic effect than in those without neurodiagnostic abnormalities (OR 4.11, 95%CI 1.88-9.02). In those with normal neurodiagnostic studies (n = 43), IVIg was effective in 14 of 17 (82%) patients as well although other immunotherapies were uniformly ineffective., Conclusions: This study reports the novel presence of neurodiagnostic testing abnormalities in individuals with Down syndrome regression disorder, providing credence to this symptom cluster potentially being of neurologic and/or neuroimmunologic etiology., (© 2022. The Author(s).)

Published

2022

6. A Community-Based Participatory Research Approach to Hurricane Katrina: When Disasters, Environmental Health Threats, and Disparities Collide.

Author

Lichtveld M, Covert H, El-Dahr J, Grimsley LF, Cohn R, Watson CH, Thornton E, and Kennedy S

Subjects

Asthma ethnology, Asthma etiology, Child, Child, Preschool, Cyclonic Storms, Fungi, Health Status Disparities, Housing, Humans, New Orleans, Asthma epidemiology, Community-Based Participatory Research, Disasters, Environmental Exposure adverse effects, Environmental Health

Abstract

In 2005, Hurricane Katrina resulted in long-term flooding of 80% of New Orleans, Louisiana. Mold-infested homes gave rise to concerns about increased childhood asthma. To address these concerns, a diverse community-academic partnership used a community-based participatory research (CBPR) approach to implement the Head-off Environmental Asthma in Louisiana (HEAL) study in 2007.The study examined the relationship between post-Katrina mold and other environmental exposures and asthma morbidity, while testing an asthma counselor (AC) intervention. Both the AC intervention and the CBPR approach were effectively implemented in the postdisaster setting. However, homes had lower levels of mold and other allergens than expected, possibly because of the timing of environmental sampling. Also, HEAL illustrated the vulnerability of the study community, especially to the interconnected threats of health disparities, environmental health stressors, and disasters.We examine the implications of these threats for public health science, policy, and practice, not only through the lens of Hurricane Katrina but also for future disasters faced by communities in the Gulf Coast and nationally.

Published

2020

7. An Unusual Cause of Frequent, Sudden, Transient, Unexplained Falls and New-Onset Status Epilepticus: Case Report and Mini-Review.

Author

Singh D, Dyer A, Gu S, McCarville P, Hess A, Akingbola O, El-Dahr J, and Nelson S

Subjects

Adolescent, Diagnosis, Differential, Electroencephalography methods, Encephalitis complications, Encephalitis diagnostic imaging, Encephalitis therapy, Female, Follow-Up Studies, Hashimoto Disease complications, Hashimoto Disease diagnostic imaging, Hashimoto Disease therapy, Humans, Intensive Care Units, Pediatric, Magnetic Resonance Angiography methods, Magnetic Resonance Imaging methods, Rare Diseases, Risk Assessment, Seizures diagnosis, Seizures therapy, Severity of Illness Index, Status Epilepticus complications, Status Epilepticus diagnostic imaging, Status Epilepticus therapy, Accidental Falls statistics & numerical data, Encephalitis diagnosis, Hashimoto Disease diagnosis, Multimodal Imaging, Status Epilepticus diagnosis

Abstract

We report a 14-year old adolescent Caucasian female, who presented with frequent, sudden, transient, and unexplained falls leading to multiple serious injuries to her head and extremities requiring several visits to the emergency department. She was evaluated numerous times and imaging studies, echocardiogram, electrocardiogram, and electroencephalogram studies were all normal. She eventually presented to outside emergency department with dystonic posturing and status epilepticus and was transferred to our pediatric intensive care unit for further management. She was diagnosed with an uncommon, underrecognized and underdiagnosed condition. To our knowledge there is no such previous report in a pediatric patient.

Published

2018

8. From Design to Dissemination: Implementing Community-Based Participatory Research in Postdisaster Communities.

Author

Lichtveld M, Kennedy S, Krouse RZ, Grimsley F, El-Dahr J, Bordelon K, Sterling Y, White L, Barlow N, DeGruy S, Paul D, Denham S, Hayes C, Sanders M, Mvula MM, Thornton E, Chulada P, Mitchell H, Martin WJ 2nd, Stephens KU, and Cohn RD

Subjects

Capacity Building organization & administration, Communication, Cyclonic Storms, Environment, Female, Health Status, Humans, Interinstitutional Relations, Louisiana, Male, Socioeconomic Factors, Community-Based Participatory Research organization & administration, Disasters, Research Design

Abstract

Objectives: To review how disasters introduce unique challenges to conducting population-based research and community-based participatory research (CBPR)., Methods: From 2007-2009, we conducted the Head-off Environmental Asthma in Louisiana (HEAL) Study in the aftermath of Hurricane Katrina in a Gulf Coast community facing an unprecedented triple burden: Katrina's and other disasters' impact on the environment and health, historic health disparities, and persistent environmental health threats., Results: The unique triple burden influenced every research component; still, most existing CBPR principles were applicable, even though full adherence was not always feasible and additional tailored principles govern postdisaster settings., Conclusions: Even in the most challenging postdisaster conditions, CBPR can be successfully designed, implemented, and disseminated while adhering to scientific rigor.

Published

2016

9. A case of invasive Streptococcus pneumoniae in an afebrile adolescent with sickle cell disease.

Author

Santoro JD, Case AE, El-Dahr J, and Kanter J

Subjects

Adolescent, Bacteremia complications, Humans, Male, Meningitis, Pneumococcal complications, Anemia, Sickle Cell complications, Bacteremia diagnosis, Meningitis, Pneumococcal diagnosis

Published

2013

10. The Head-off Environmental Asthma in Louisiana (HEAL) study--methods and study population.

Author

Chulada PC, Kennedy S, Mvula MM, Jaffee K, Wildfire J, Thornton E, Cohn RD, Grimsley LF, Mitchell H, El-Dahr J, Sterling Y, Martin WJ, White L, Stephens KU, and Lichtveld M

Subjects

Allergens analysis, Allergens toxicity, Asthma etiology, Child, Child, Preschool, Cyclonic Storms, Disasters, Female, Housing, Humans, Male, Morbidity, New Orleans epidemiology, Research Design, Socioeconomic Factors, Asthma epidemiology, Environmental Exposure, Health Surveys methods

Abstract

Background: In the city of New Orleans, Louisiana, and surrounding parishes (NOLA), children with asthma were perilously impacted by Hurricane Katrina as a result of disrupted health care, high home mold and allergen levels, and high stress., Objectives: The Head-off Environmental Asthma in Louisiana (HEAL) study was conducted to examine relationships between the post-Katrina environment and childhood asthma in NOLA and assess a novel asthma counselor intervention that provided case management and guidance for reducing home mold and allergen levels., Methods: Children (4-12 years old) with moderate-to-severe asthma were recruited from NOLA schools. Over 1 year, they received two clinical evaluations, three home environmental evaluations, and the asthma intervention. Quarterly end points included symptom days, medication use, and unscheduled emergency department or clinic visits. A community advisory group was assembled and informed HEAL at all phases., Results: Of the children (n = 182) enrolled in HEAL, 67% were African American, and 25% came from households with annual incomes < $15,000. HEAL children were symptomatic, averaging 6.6 symptom days in the 2 weeks before baseline, and had frequent unscheduled visits to clinics or emergency departments (76% had at least one unscheduled visit in the preceding 3 months). In this report, we describe study design and baseline characteristics of HEAL children., Conclusions: Despite numerous challenges faced by investigators, study staff, and participants, including destroyed infrastructure, disrupted lives, and lost jobs, HEAL was successful in terms of recruitment and retention, the high quality of data collected that will provide insight into asthma-allergen relationships, and the asthma intervention. This success was attributable to using an adaptive approach and refining processes as needed.

Published

2012

11. Indoor environmental exposures for children with asthma enrolled in the HEAL study, post-Katrina New Orleans.

Author

Grimsley LF, Chulada PC, Kennedy S, White L, Wildfire J, Cohn RD, Mitchell H, Thornton E, El-Dahr J, Mvula MM, Sterling Y, Martin WJ, Stephens KU, and Lichtveld M

Subjects

Air Pollutants toxicity, Air Pollution, Indoor adverse effects, Allergens adverse effects, Asthma etiology, Child, Child, Preschool, Cyclonic Storms, Disasters, Environmental Monitoring, Enzyme-Linked Immunosorbent Assay, Female, Housing, Humans, Male, Morbidity, New Orleans epidemiology, Air Pollutants analysis, Air Pollution, Indoor analysis, Allergens analysis, Asthma epidemiology, Dust analysis, Environmental Exposure

Abstract

Background: Rain and flooding from Hurricane Katrina resulted in widespread growth of mold and bacteria and production of allergens in New Orleans, Louisiana, which may have led to increased exposures and morbidity in children with asthma., Objectives: The goal of the Head-off Environmental Asthma in Louisiana (HEAL) study was to characterize post-Katrina exposures to mold and allergens in children with asthma., Methods: The homes of 182 children with asthma in New Orleans and surrounding parishes were evaluated by visual inspection, temperature and moisture measurements, and air and dust sampling. Air was collected using vacuum-pump spore traps and analyzed for > 30 mold taxa using bright field microscopy. Dust was collected from the children's beds and bedroom floors and analyzed for mouse (Mus m 1), dust mite (Der p 1), cockroach (Bla g 1), and mold (Alternaria mix) allergens using ELISA., Results: More than half (62%) of the children were living in homes that had been damaged by rain, flooding, or both. Geometric mean indoor and outdoor airborne mold levels were 501 and 3,958 spores/m3, respectively. Alternaria antigen was detected in dust from 98% of homes, with 58% having concentrations > 10 µg/g. Mus m 1, Der p 1, and Bla g 1 were detected in 60%, 35%, and 20% of homes, respectively, at low mean concentrations., Conclusions: Except for Alternaria antigen in dust, concentrations of airborne mold (ratio of indoor to outdoor mold) and dust allergens in the homes of HEAL children were lower than measurements found in other studies, possibly because of extensive post-Katrina mold remediation and renovations, or because children moved into cleaner homes upon returning to New Orleans.

Published

2012

12. Safety and efficacy of oral DMSA therapy for children with autism spectrum disorders: Part A--medical results.

Author

Adams JB, Baral M, Geis E, Mitchell J, Ingram J, Hensley A, Zappia I, Newmark S, Gehn E, Rubin RA, Mitchell K, Bradstreet J, and El-Dahr J

Subjects

Administration, Oral, Autistic Disorder blood, Autistic Disorder urine, Blood Cell Count methods, Child, Child, Preschool, Double-Blind Method, Female, Glutathione blood, Glutathione urine, Humans, Male, Metals blood, Metals urine, Treatment Outcome, Autistic Disorder drug therapy, Succimer administration & dosage, Succimer adverse effects

Abstract

Background: This study investigated the effect of oral dimercapto succinic acid (DMSA) therapy for children with autism spectrum disorders ages 3-8 years., Methods: Phase 1 involved 65 children who received one round of DMSA (3 days). Participants who had high urinary excretion of toxic metals were selected to continue on to phase 2. In phase 2, 49 participants were randomly assigned in a double-blind design to receive an additional 6 rounds of either DMSA or placebo., Results: DMSA greatly increased the excretion of lead, substantially increased excretion of tin and bismuth, and somewhat increased the excretion of thallium, mercury, antimony, and tungsten. There was some increase in urinary excretion of essential minerals, especially potassium and chromium. The Phase 1 single round of DMSA led to a dramatic normalization of RBC glutathione in almost all cases, and greatly improved abnormal platelet counts, suggesting a significant decrease in inflammation., Conclusion: Overall, DMSA therapy seems to be reasonably safe, effective in removing several toxic metals (especially lead), dramatically effective in normalizing RBC glutathione, and effective in normalizing platelet counts. Only 1 round (3 days) was sufficient to improve glutathione and platelets. Additional rounds increased excretion of toxic metals.

Published

2009

13. Safety and efficacy of oral DMSA therapy for children with autism spectrum disorders: part B - behavioral results.

Author

Adams JB, Baral M, Geis E, Mitchell J, Ingram J, Hensley A, Zappia I, Newmark S, Gehn E, Rubin RA, Mitchell K, Bradstreet J, and El-Dahr J

Subjects

Aging, Autistic Disorder classification, Autistic Disorder complications, Child, Child, Preschool, Drug Administration Schedule, Glutathione blood, Heavy Metal Poisoning, Nervous System complications, Humans, Metals, Heavy toxicity, Metals, Heavy urine, Parents psychology, Psychiatric Status Rating Scales, Regression Analysis, Surveys and Questionnaires, Treatment Outcome, Adaptation, Psychological drug effects, Autistic Disorder drug therapy, Chelating Agents adverse effects, Chelating Agents therapeutic use, Child Behavior drug effects, Succimer adverse effects, Succimer therapeutic use

Abstract

Background: This study investigated the effects of oral dimercapto succinic acid (DMSA) therapy on the behavioural symptoms of children with autism spectrum disorders (ASD) ages 3-8 years., Methods: Phase 1 involved 65 children with ASD who received one round of DMSA (3 days). Participants who had high urinary excretion of toxic metals were selected to continue on to phase 2. In phase 2, 49 participants were randomly assigned in a double-blind design to receive an additional 6 rounds of either DMSA or placebo., Results: The groups receiving one round and seven rounds of DMSA had significant improvements on all the assessment measures. For the seven round group, the degree of improvement on the assessment measures could be partially explained by a regression analysis based on excretion of toxic metals and changes in glutathione (adjusted R2 of 0.28-0.75, p < 0.02 in all cases). One round of DMSA had nearly the same benefit as seven rounds. The assessment measures correlated reasonably with one another at the beginning of the study (r = 0.60-0.87) and even better at the end of the study (r = 0.63-0.94)., Conclusion: Overall, both one and seven rounds of DMSA therapy seems to be reasonably safe in children with ASD who have high urinary excretion of toxic metals, and possibly helpful in reducing some of the symptoms of autism in those children.

Published

2009

14. Prevalence of IgE reactivities in mold-allergic subjects to commercially available fungal enzymes.

Author

Horner WE, Armstrong M, El-Dahr J, McCants M, Reese G, Kobernick AK, and Lehrer SB

Subjects

Cellulase immunology, Fungi enzymology, Glucosidases immunology, Humans, Respiratory Hypersensitivity microbiology, Saccharomyces cerevisiae enzymology, Saccharomyces cerevisiae immunology, Trichoderma enzymology, Trichoderma immunology, beta-Fructofuranosidase immunology, Allergens immunology, Antibodies, Fungal blood, Antigens, Fungal immunology, Enzymes immunology, Fungi immunology, Immunoglobulin E blood, Respiratory Hypersensitivity immunology

Abstract

Fungi are important aeroallergens. However, fungal allergen sources of consistent quality for clinical testing are not readily available. Because some allergens have been identified as enzymes, we assessed the prevalence of IgE reactivity to commercially available fungal enzymes. The purpose of this study was to determine IgE antibody reactivity by radioallergosorbent assay (RAST) to commercially available fungal enzymes in mold-allergic individuals. Sera from 20 subjects with symptoms of respiratory allergies and skin test reactivity to 2 or more fungal allergens (4 conidial [imperfecti] fungi and/or 8 basidiomycetes) were selected. Controls were six atopic individuals with neither history of fungal allergy nor skin test reactivity to fungi. Seventeen commercial fungal enzymes were used as antigens to evaluate the subjects' IgE antibody reactivity by RAST. Sera from most fungus-allergic individuals showed substantial IgE antibody reactivity to enzymes; control sera showed little or no reactivity. The mean reactivity to all commercial enzymes of all subjects tested was RAST > or = 3% with only one exception. The most reactive fungal enzymes were invertase (bakers' yeast, Saccharomyces cerevisiae), cellulase (Trichoderma viride), and glucosidase (brewers yeast, S. cerevisiae) with mean binding of 14.6, 9.5, and 8.8%, respectively. Using RAST results with a combination of four enzymes from S. cerevisiae (brewers yeast glucosidase, bakers' yeast maltase, invertase, and invertase V), a sensitivity of 100% was shown for detecting mold-allergic patients. The studies suggest that fungal enzymes may be useful source materials for the identification of fungal allergens and may also provide readily available source materials to produce improved diagnostic and therapeutic reagents.

Published

2008

15. Fish allergy: is cross-reactivity among fish species relevant? Double-blind placebo-controlled food challenge studies of fish allergic adults.

Author

Helbling A, Haydel R Jr, McCants ML, Musmand JJ, El-Dahr J, and Lehrer SB

Subjects

Adult, Animals, Cross Reactions immunology, Double-Blind Method, Erythema immunology, Female, Humans, Male, Mouth Diseases immunology, Radioallergosorbent Test, Skin Tests, Species Specificity, Fishes immunology, Food Hypersensitivity immunology

Abstract

Background: Allergic reactions to fish are a common cause of food allergy in many areas of the world where fish is a major source of protein. Although different species of fish may be consumed, possible cross-reactivity has received limited investigation., Objective: The aim of this study was to assess potential cross-reactivity to different species of fish species using double-blind, placebo-controlled food challenges (DBPCFC) in fish-allergic adults and to compare skin test and RAST reactivity with the challenge response., Methods: Nine skin prick test and/or RAST-positive adult individuals with histories of an immediate-type reaction following fish ingestion were challenged with different fish species using double-blind, placebo-controlled food challenge., Results: Of a total of 19 double-blind, placebo-controlled fish challenges performed, 14 challenges (74%) resulted in the induction of objective signs that were consistent with an IgE-mediated response. The most common sign observed was emesis (37%); the most prevalent subjective symptoms reported were compatible with the oral allergy syndrome (84%). Three subjects reacted to at least three fish species and one subject reacted to two fish species tested. In regard to the positive challenges, predictive accuracy of skin prick test and RAST was 84% and 78%, respectively., Conclusion: Our results indicate that clinically relevant cross-reactivity among various species of fish may exist. Advising fish-allergic subjects to avoid all fish species should be emphasized until a species can be proven safe to eat by provocative challenge.

Published

1999

16. Seven novel mutations in the adenosine deaminase (ADA) gene in patients with severe and delayed onset combined immunodeficiency: G74C, V129M, G140E, R149W, Q199P, 462delG, and E337del. Mutations in brief no. 142. Online.

Author

Arrendondo-Vega FX, Santisteban I, Notarangelo LD, El Dahr J, Buckley R, Roifman C, Conley ME, and Hershfield MS

Subjects

Adenosine Deaminase deficiency, Adolescent, Adult, Age of Onset, Arginine genetics, Cysteine genetics, Glutamic Acid genetics, Glutamine genetics, Glycine genetics, Humans, Methionine genetics, Proline genetics, Sequence Deletion genetics, Tryptophan genetics, Valine genetics, Adenosine Deaminase genetics, Mutation genetics, Severe Combined Immunodeficiency genetics

Abstract

The degree of immunodeficiency associated with deficiency of adenosine deaminase (ADA) is variable. Most patients are infants with severe combined immunodeficiency (SCID), but in about 20 percent immune dysfunction becomes manifest later in childhood ("delayed-onset"); several patients with "late" or "adult" onset of immune dysfunction have been diagnosed at 15-39 years. Over 40 ADA gene mutations have thus far been identified. To better define the genotype-phenotype relationship, we report 7 novel ADA mutations, including 5 missense mutations (G74C, V129M, G140E, R149W, Q199P) and two short deletions (462delG, E337del). These were identified among 7 patients (3 with SCID and 4 with delayed-onset). A homozygote for 462delG had SCID, whereas patients homozygous or heterozyous for V129M had delayed-onset. Two other delayed-onset patients, one heterozygous for G74C and the other for Q199P, each had a second allele carrying the previously reported "severe" mutation G216R. These findings are consistent with previous observations suggesting that, in general, SCID occurs when both alleles eliminate ADA function, and a milder phenotype when at least one allele can supply a low level of function.

Published

1998

17. Failure to thrive, diarrhea, cough, and oral candidiasis in a three-month-old boy.

Author

Walcott DW, Linehan T 4th, Hilman BC, Hershfield MS, and el Dahr J

Subjects

Acquired Immunodeficiency Syndrome diagnosis, Adenosine Deaminase therapeutic use, Animals, Cystic Fibrosis diagnosis, Diagnosis, Differential, Follow-Up Studies, Humans, Infant, Male, Rabbits, Severe Combined Immunodeficiency complications, Wiskott-Aldrich Syndrome diagnosis, Adenosine Deaminase deficiency, Candidiasis, Oral complications, Cough complications, Diarrhea complications, Failure to Thrive complications, Severe Combined Immunodeficiency diagnosis

Published

1994