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1. NFKB2 haploinsufficiency identified via screening for IFN-α2 autoantibodies in children and adolescents hospitalized with SARS-CoV-2–related complications

Author

Bodansky, Aaron, Vazquez, Sara E, Chou, Janet, Novak, Tanya, Al-Musa, Amer, Young, Cameron, Newhams, Margaret, Kucukak, Suden, Zambrano, Laura D, Mitchell, Anthea, Wang, Chung-Yu, Moffitt, Kristin, Halasa, Natasha B, Loftis, Laura L, Schwartz, Stephanie P, Walker, Tracie C, Mack, Elizabeth H, Fitzgerald, Julie C, Gertz, Shira J, Rowan, Courtney M, Irby, Katherine, Sanders, Ronald C, Kong, Michele, Schuster, Jennifer E, Staat, Mary A, Zinter, Matt S, Cvijanovich, Natalie Z, Tarquinio, Keiko M, Coates, Bria M, Flori, Heidi R, Dahmer, Mary K, Crandall, Hillary, Cullimore, Melissa L, Levy, Emily R, Chatani, Brandon, Nofziger, Ryan, Investigators, Overcoming COVID-19 Network Study Group, Yates, Masson, Smith, Chelsea, Zinter, MattS, McLaughlin, Gwenn, Randolph, Adrienne G, Newhams, Margaret M, Moon, Hye Kyung, Kobayashi, Takuma, Melo, Jeni, Chen, Sabrina R, Behl, Supriya, Drapeau, Noelle M, McCulloh, Russell J, Nofziger, Ryan A, Staat, Mary Allen, Rohlfs, Chelsea C, Reed, Nelson, Geha, Raif S, DeRisi, Joseph, Campbell, Angela P, and Anderson, Mark

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, Vaccine Related, Infectious Diseases, Rare Diseases, Pneumonia, Clinical Research, Prevention, Emerging Infectious Diseases, Biodefense, Pediatric, Genetics, Autoimmune Disease, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Good Health and Well Being, Adult, Humans, Child, Adolescent, SARS-CoV-2, COVID-19, Autoantibodies, NF-kappa B, Haploinsufficiency, Leukocytes, Mononuclear, Interferon Type I, NF-kappa B p52 Subunit, Anti-interferon autoantibody, MIS-C, NFKB2, inborn errors of immunity, Overcoming COVID-19 Network Study Group Investigators, Immunology, Allergy
Abstract

BackgroundAutoantibodies against type I IFNs occur in approximately 10% of adults with life-threatening coronavirus disease 2019 (COVID-19). The frequency of anti-IFN autoantibodies in children with severe sequelae of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection is unknown.ObjectiveWe quantified anti-type I IFN autoantibodies in a multicenter cohort of children with severe COVID-19, multisystem inflammatory syndrome in children (MIS-C), and mild SARS-CoV-2 infections.MethodsCirculating anti-IFN-α2 antibodies were measured by a radioligand binding assay. Whole-exome sequencing, RNA sequencing, and functional studies of peripheral blood mononuclear cells were used to study any patients with levels of anti-IFN-α2 autoantibodies exceeding the assay's positive control.ResultsAmong 168 patients with severe COVID-19, 199 with MIS-C, and 45 with mild SARS-CoV-2 infections, only 1 had high levels of anti-IFN-α2 antibodies. Anti-IFN-α2 autoantibodies were not detected in patients treated with intravenous immunoglobulin before sample collection. Whole-exome sequencing identified a missense variant in the ankyrin domain of NFKB2, encoding the p100 subunit of nuclear factor kappa-light-chain enhancer of activated B cells, aka NF-κB, essential for noncanonical NF-κB signaling. The patient's peripheral blood mononuclear cells exhibited impaired cleavage of p100 characteristic of NFKB2 haploinsufficiency, an inborn error of immunity with a high prevalence of autoimmunity.ConclusionsHigh levels of anti-IFN-α2 autoantibodies in children and adolescents with MIS-C, severe COVID-19, and mild SARS-CoV-2 infections are rare but can occur in patients with inborn errors of immunity.

Published
2023

3. Regulatory T-cell dysfunction and cutaneous exposure to Staphylococcus aureus underlie eczema in DOCK8 deficiency

Author

Wilkie, Hazel, Das, Mrinmoy, Pelovitz, Tyler, Bainter, Wayne, Woods, Brian, Alasharee, Mohammed, Sobh, Ali, Baris, Safa, Eltan, Sevgi Bilgic, Al-Herz, Waleed, Barbouche, Mohamed-Ridha, Ben-Mustapha, Imen, Ben-Ali, Meriem, Sallam, Mohamed T.H., Awad, Amany, Lotfy, Sohilla, El Marsafy, Aisha, Ezzelarab, Moushira, Farrar, Michael, Schmidt, Brigitta A.R., NandyMazumdar, Monali, Guttman-Yassky, Emma, Sheets, Anthony, Vidic, Katie Maria, Murphy, George, Schlievert, Patrick M., Chou, Janet, Leyva-Castillo, Juan Manuel, Janssen, Erin, Timilshina, Maheshwor, and Geha, Raif S.

Published
2024
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8. The IL-4Rα Q576R polymorphism is associated with increased severity of atopic dermatitis and exaggerates allergic skin inflammation in mice

Author

Yang, Barbara, Wilkie, Hazel, Das, Mrinmoy, Timilshina, Maheshwor, Bainter, Wayne, Woods, Brian, Daya, Michelle, Boorgula, Meher P., Mathias, Rasika A., Lai, Peggy, Petty, Carter R., Weller, Edie, Harb, Hani, Chatila, Talal A., Leung, Donald Y.M., Beck, Lisa A., Simpson, Eric L., Hata, Tissa R., Barnes, Kathleen C., Phipatanakul, Wanda, Leyva-Castillo, Juan-Manuel, and Geha, Raif S.

Published
2023
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9. Outcomes and Treatment Strategies for Autoimmunity and Hyperinflammation in Patients with RAG Deficiency

Author

Farmer, Jocelyn R, Foldvari, Zsofia, Ujhazi, Boglarka, De Ravin, Suk See, Chen, Karin, Bleesing, Jack JH, Schuetz, Catharina, Al-Herz, Waleed, Abraham, Roshini S, Joshi, Avni Y, Costa-Carvalho, Beatriz T, Buchbinder, David, Booth, Claire, Reiff, Andreas, Ferguson, Polly J, Aghamohammadi, Asghar, Abolhassani, Hassan, Puck, Jennifer M, Adeli, Mehdi, Cancrini, Caterina, Palma, Paolo, Bertaina, Alice, Locatelli, Franco, Di Matteo, Gigliola, Geha, Raif S, Kanariou, Maria G, Lycopoulou, Lilia, Tzanoudaki, Marianna, Sleasman, John W, Parikh, Suhag, Pinero, Gloria, Fischer, Bernard M, Dbaibo, Ghassan, Unal, Ekrem, Patiroglu, Turkan, Karakukcu, Musa, Al-Saad, Khulood Khalifa, Dilley, Meredith A, Pai, Sung-Yun, Dutmer, Cullen M, Gelfand, Erwin W, Geier, Christoph B, Eibl, Martha M, Wolf, Hermann M, Henderson, Lauren A, Hazen, Melissa M, Bonfim, Carmem, Wolska-Kuśnierz, Beata, Butte, Manish J, Hernandez, Joseph D, Nicholas, Sarah K, Stepensky, Polina, Chandrakasan, Shanmuganathan, Miano, Maurizio, Westermann-Clark, Emma, Goda, Vera, Kriván, Gergely, Holland, Steven M, Fadugba, Olajumoke, Henrickson, Sarah E, Ozen, Ahmet, Karakoc-Aydiner, Elif, Baris, Safa, Kiykim, Ayca, Bredius, Robbert, Hoeger, Birgit, Boztug, Kaan, Pashchenko, Olga, Neven, Benedicte, Moshous, Despina, Villartay, Jean-Pierre de, Bousfiha, Ahmed Aziz, Hill, Harry R, Notarangelo, Luigi D, and Walter, Jolan E

Subjects
Autoimmune Disease, Genetics, Hematology, Inflammatory and immune system, Adolescent, Adult, Autoimmunity, Child, Child, Preschool, Female, Hematopoietic Stem Cell Transplantation, Homeodomain Proteins, Humans, Immunologic Deficiency Syndromes, Immunosuppressive Agents, Infant, Inflammation, Male, Middle Aged, Treatment Outcome, Young Adult, Recombination activating gene, Severe combined immunodeficiency, Immune dysregulation, Autoimmune cytopenias, Hematopoietic stem cell transplantation
Abstract

BACKGROUND:Although autoimmunity and hyperinflammation secondary to recombination activating gene (RAG) deficiency have been associated with delayed diagnosis and even death, our current understanding is limited primarily to small case series. OBJECTIVE:Understand the frequency, severity, and treatment responsiveness of autoimmunity and hyperinflammation in RAG deficiency. METHODS:In reviewing the literature and our own database, we identified 85 patients with RAG deficiency, reported between 2001 and 2016, and compiled the largest case series to date of 63 patients with prominent autoimmune and/or hyperinflammatory pathology. RESULTS:Diagnosis of RAG deficiency was delayed a median of 5 years from the first clinical signs of immune dysregulation. Most patients (55.6%) presented with more than 1 autoimmune or hyperinflammatory complication, with the most common etiologies being cytopenias (84.1%), granulomas (23.8%), and inflammatory skin disorders (19.0%). Infections, including live viral vaccinations, closely preceded the onset of autoimmunity in 28.6% of cases. Autoimmune cytopenias had early onset (median, 1.9, 2.1, and 2.6 years for autoimmune hemolytic anemia, immune thrombocytopenia, and autoimmune neutropenia, respectively) and were refractory to intravenous immunoglobulin, steroids, and rituximab in most cases (64.7%, 73.7%, and 71.4% for autoimmune hemolytic anemia, immune thrombocytopenia, and autoimmune neutropenia, respectively). Evans syndrome specifically was associated with lack of response to first-line therapy. Treatment-refractory autoimmunity/hyperinflammation prompted hematopoietic stem cell transplantation in 20 patients. CONCLUSIONS:Autoimmunity/hyperinflammation can be a presenting sign of RAG deficiency and should prompt further evaluation. Multilineage cytopenias are often refractory to immunosuppressive treatment and may require hematopoietic cell transplantation for definitive management.

Published
2019

10. Clinical, immunological, molecular and therapeutic findings in monogenic immune dysregulation diseases: Middle East and North Africa registry

Author

Rasouli, Seyed Erfan, Esmaeili, Marzie, Yazdani, Reza, Delavari, Samaneh, Tavakol, Marzieh, Sadri, Homa, Karimi, Abdollah, Shiari, Reza, Alavi, Samin, Babaie, Delara, Eshghi, Peyman, Armin, Shahnaz, Vosughimotlagh, Ahmad, Eltan, Sevgi Bilgic, Babayeva, Royala, Sefer, Asena Pinar, Kolukisa, Burcu, Gungoren, Ezgi Yalcin, Altunbas, Melek Yorgun, Mammadova, Vafa, Jamee, Mahnaz, Azizi, Gholamreza, Baris, Safa, Karakoc-Aydiner, Elif, Ozen, Ahmet, Kiliç, Sara Ş., Kose, Hulya, Chavoshzadeh, Zahra, Mahdaviani, Seyed Alireza, Momen, Tooba, Shamsian, Bibi Shahin, Fallahi, Mazdak, Sharafian, Samin, Gülez, Nesrin, Aygun, Ayşe, Karaca, Neslihan Edeer, Kutukculer, Necil, Al Sukait, Nashat, Al Farsi, Tariq, Al-Tamemi, Salem, Khalifa, Nisreen, Shereen, Reda, El-Ghoneimy, Dalia, El-Owaidy, Rasha, Radwan, Nesrine, Alzyoud, Raed, Barbouche, Mohamed-Ridha, Ben-Mustapha, Imen, Mekki, Najla, Rais, Afef, Boukari, Rachida, Belbouab, Reda, Djenouhat, Kamel, Tahiat, Azzeddine, Touri, Souad, Elghazali, Gehad, Al-Hammadi, Suleiman, Shendi, Hiba Mohammed, Alkuwaiti, Amna, Belaid, Brahim, Djidjik, Reda, Artac, Hasibe, Adeli, Mehdi, Sobh, Ali, Elnagdy, Marwa H., Bahgat, Sara A., Nasrullayeva, Gulnara, Chou, Janet, Rezaei, Nima, Al-Herz, Waleed, Geha, Raif S., and Abolhassani, Hassan

Published
2022
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12. The Middle East and North Africa Diagnosis and Management Guidelines for Inborn Errors of Immunity

Author

Baris, Safa, Abolhassani, Hassan, Massaad, Michel J., Al-Nesf, Maryam, Chavoshzadeh, Zahra, Keles, Sevgi, Reisli, Ismail, Tahiat, Azzeddine, Shendi, Hiba Mohammad, Elaziz, Dalia Abd, Belaid, Brahim, Al Dhaheri, Fatima, Haskologlu, Sule, Dogu, Figen, Ben-Mustapha, Imen, Sobh, Ali, Galal, Nermeen, Meshaal, Safa, Elhawary, Rabab, El-marsafy, Aisha, Alroqi, Fayhan J., Al-Saud, Bandar, Al-Ahmad, Mona, Al Farsi, Tariq, AL Sukaiti, Nashat, Al-Tamemi, Salem, Mehawej, Cybel, Dbaibo, Ghassan, ElGhazali, Gehad, Kilic, Sara Sebnem, Genel, Ferah, Kiykim, Ayca, Musabak, Ugur, Artac, Hasibe, Guner, Sukru Nail, Boukari, Rachida, Djidjik, Reda, Kechout, Nadia, Cagdas, Deniz, El-Sayed, Zeinab Awad, Karakoc-Aydiner, Elif, Alzyoud, Raed, Barbouche, Mohamed Ridha, Adeli, Mehdi, Wakim, Rima Hanna, Reda, Shereen M., Ikinciogullari, Aydan, Ozen, Ahmet, Bousfiha, Aziz, Al-Mousa, Hamoud, Rezaei, Nima, Al-Herz, Waleed, and Geha, Raif S.

Published
2022
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13. Mechanisms of genotype-phenotype correlation in autosomal dominant anhidrotic ectodermal dysplasia with immune deficiency

Author

Petersheim, Daniel, Massaad, Michel J, Lee, Saetbyul, Scarselli, Alessia, Cancrini, Caterina, Moriya, Kunihiko, Sasahara, Yoji, Lankester, Arjan C, Dorsey, Morna, Di Giovanni, Daniela, Bezrodnik, Liliana, Ohnishi, Hidenori, Nishikomori, Ryuta, Tanita, Kay, Kanegane, Hirokazu, Morio, Tomohiro, Gelfand, Erwin W, Jain, Ashish, Secord, Elizabeth, Picard, Capucine, Casanova, Jean-Laurent, Albert, Michael H, Torgerson, Troy R, and Geha, Raif S

Subjects
Genetics, Aetiology, 2.1 Biological and endogenous factors, Carrier Proteins, Chemokine CCL20, Ectodermal Dysplasia, Genetic Diseases, X-Linked, Genotype, HEK293 Cells, Humans, Immunologic Deficiency Syndromes, Intercellular Adhesion Molecule-1, Interleukin-6, NF-KappaB Inhibitor alpha, NF-kappa B p52 Subunit, Point Mutation, Primary Immunodeficiency Diseases, Proto-Oncogene Mas, Signal Transduction, Ectodermal dysplasia with immune deficiency, NF-kappa B inhibitor alpha, canonical nuclear factor kappa B pathway, noncanonical nuclear factor kappa B pathway, lymphorganogenesis, hematopoietic stem cell transplantation, NF-κB inhibitor α, canonical nuclear factor κB pathway, noncanonical nuclear factor κB pathway, Immunology, Allergy
Abstract

BackgroundAutosomal dominant anhidrotic ectodermal dysplasia with immune deficiency (AD EDA-ID) is caused by heterozygous point mutations at or close to serine 32 and serine 36 or N-terminal truncations in IκBα that impair its phosphorylation and degradation and thus activation of the canonical nuclear factor κ light chain enhancer of activated B cells (NF-κB) pathway. The outcome of hematopoietic stem cell transplantation is poor in patients with AD EDA-ID despite achievement of chimerism. Mice heterozygous for the serine 32I mutation in IκBα have impaired noncanonical NF-κB activity and defective lymphorganogenesis.ObjectiveWe sought to establish genotype-phenotype correlation in patients with AD EDA-ID.MethodsA disease severity scoring system was devised. Stability of IκBα mutants was examined in transfected cells. Immunologic, biochemical, and gene expression analyses were performed to evaluate canonical and noncanonical NF-κB signaling in skin-derived fibroblasts.ResultsDisease severity was greater in patients with IκBα point mutations than in those with truncation mutations. IκBα point mutants were expressed at significantly higher levels in transfectants compared with truncation mutants. Canonical NF-κB-dependent IL-6 secretion and upregulation of the NF-κB subunit 2/p100 and RELB proto-oncogene, NF-κB subunit (RelB) components of the noncanonical NF-κB pathway were diminished significantly more in patients with point mutations compared with those with truncations. Noncanonical NF-κB-driven generation of the transcriptionally active p100 cleavage product p52 and upregulation of CCL20, intercellular adhesion molecule 1 (ICAM1), and vascular cell adhesion molecule 1 (VCAM1), which are important for lymphorganogenesis, were diminished significantly more in LPS plus α-lymphotoxin β receptor-stimulated fibroblasts from patients with point mutations compared with those with truncations.ConclusionsIκBα point mutants accumulate at higher levels compared with truncation mutants and are associated with more severe disease and greater impairment of canonical and noncanonical NF-κB activity in patients with AD EDA-ID.

Published
2018

17. Multi-kingdom ecological drivers of microbiota assembly in preterm infants

Author

Rao, Chitong, Coyte, Katharine Z., Bainter, Wayne, Geha, Raif S., Martin, Camilia R., and Rakoff-Nahoum, Seth

Subjects
Microbiota (Symbiotic organisms) -- Growth, Ecosystem components -- Physiological aspects, Host-bacteria relationships -- Analysis, Infants (Premature) -- Contamination -- Health aspects, Company growth, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

The gut microbiota of preterm infants develops predictably.sup.1-7, with pioneer species colonizing the gut after birth, followed by an ordered succession of microorganisms. The gut microbiota is vital to the health of preterm infants.sup.8,9, but the forces that shape these predictable dynamics of microbiome assembly are unknown. The environment, the host and interactions between microorganisms all potentially shape the dynamics of the microbiota, but in such a complex ecosystem, identifying the specific role of any individual factor is challenging.sup.10-14. Here we use multi-kingdom absolute abundance quantification, ecological modelling and experimental validation to address this challenge. We quantify the absolute dynamics of bacteria, fungi and archaea in a longitudinal cohort of 178 preterm infants. We uncover microbial blooms and extinctions, and show that there is an inverse correlation between bacterial and fungal loads in the infant gut. We infer computationally and demonstrate experimentally in vitro and in vivo that predictable assembly dynamics may be driven by directed, context-dependent interactions between specific microorganisms. Mirroring the dynamics of macroscopic ecosystems.sup.15-17, a late-arriving member of the microbiome, Klebsiella, exploits the pioneer microorganism, Staphylococcus, to gain a foothold within the gut. Notably, we find that interactions between different kingdoms can influence assembly, with a single fungal species--Candida albicans--inhibiting multiple dominant genera of gut bacteria. Our work reveals the centrality of simple microbe-microbe interactions in shaping host-associated microbiota, which is critical both for our understanding of microbiota ecology and for targeted microbiota interventions. Absolute microbial abundances delineate longitudinal dynamics of bacteria, fungi and archaea in the infant gut microbiome, uncovering drivers of microbiome development masked by relative abundances and revealing notable parallels to macroscopic ecosystem assemblies., Author(s): Chitong Rao [sup.1] , Katharine Z. Coyte [sup.1] [sup.2] , Wayne Bainter [sup.3] , Raif S. Geha [sup.3] , Camilia R. Martin [sup.4] , Seth Rakoff-Nahoum [sup.1] [sup.5] [sup.6] [...]

Published
2021
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18. The Notch1/CD22 signaling axis disrupts Treg function in SARS-CoV-2-associated multisystem inflammatory syndrome in children

Author

Benamar, Mehdi, Chen, Qian, Chou, Janet, Jule, Amelie M., Boudra, Rafik, Contini, Paola, Crestani, Elena, Lai, Peggy S., Wang, Muyun, Fong, Jason, Rockwitz, Shira, Lee, Pui, Chan, Tsz Man Fion, Altun, Ekin Zeynep, Kepenekli, Eda, Karakoc-Aydiner, Elif, Ozen, Ahmet, Boran, Perran, Aygun, Fatih, Onal, Pinar, Sakalli, Ayse Ayzit Kilinc, Cokugras, Haluk, Gelmez, Metin Yusuf, Oktelik, Fatma Betul, Cetin, Esin Aktas, Zhong, Yuelin, Taylor, Maria Lucia, Irby, Katherine, Halasa, Natasha B., Mack, Elizabeth H., Signa, Sara, Prigione, Ignazia, Gattorno, Marco, Cotugno, Nicola, Amodio, Donato, Geha, Raif S., Son, Mary Beth, Newburger, Jane, Agrawal, Pankaj B., Volpi, Stefano, Palma, Paolo, Kiykim, Ayca, Randolph, Adrienne G., Deniz, Gunnur, Baris, Safa, De Palma, Raffaele, Schmitz-Abe, Klaus, Charbonnier, Louis-Marie, Henderson, Lauren A., and Chatila, Talal A.

Subjects
Suppressor cells -- Health aspects -- Physiological aspects, Cellular signal transduction -- Research, Pediatric research, Health care industry
Abstract

Multisystem inflammatory syndrome in children (MIS-C) evolves in some pediatric patients following acute infection with SARS-CoV-2 by hitherto unknown mechanisms. Whereas acute-COVID-19 severity and outcomes were previously correlated with Notch4 expression on Tregs, here, we show that Tregs in MIS-C were destabilized through a Notch1-dependent mechanism. Genetic analysis revealed that patients with MIS-C had enrichment of rare deleterious variants affecting inflammation and autoimmunity pathways, including dominant-negative mutations in the Notch1 regulators NUMB and NUMBL leading to Notch1 upregulation. Notch1 signaling in Tregs induced CD22, leading to their destabilization in a mTORC1dependent manner and to the promotion of systemic inflammation. These results identify a Notch1/CD22 signaling axis that disrupts Treg function in MIS-C and point to distinct immune checkpoints controlled by individual Treg Notch receptors that shape the inflammatory outcome in SARS-CoV-2 infection., Introduction COVID-19, caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), has resulted in massive morbidity and mortality worldwide (1, 2). Acute infection is associated in some individuals with [...]

Published
2023
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21. Hypomorphic variants in AK2 reveal the contribution of mitochondrial function to B-cell activation

Author

Chou, Janet, Alazami, Anas M., Jaber, Faris, Hoyos-Bachiloglu, Rodrigo, Jones, Jennifer, Weeks, Sabrina, Alosaimi, Mohammed F., Bainter, Wayne, Cangemi, Brittney, Badran, Yousef R., Mohammed, Reem, Alroqi, Fayhan, Almutairi, Abduarahman, Al-Onazi, Noufa, AlAjaji, Sulaiman, Al-Saud, Bander, Arnaout, Rand, Elkins, Megan, Devana, Sridevi, Imperial, Juliet, Li, Betty, Drexhage, Linnea, Abdel Rahman, Anas M., Jacob, Minnie, Haddad, Hadi, Hanna-Wakim, Rima, Dbaibo, Ghassan, Massaad, Michel J., Dasouki, Majed, Mikhael, Raymond, Baz, Zeina, Geha, Raif S., and Al-Mousa, Hamoud

Published
2020
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23. Genotype and functional correlates of disease phenotype in deficiency of adenosine deaminase 2 (DADA2)

Author

Lee, Pui Y., Kellner, Erinn S., Huang, Yuelong, Furutani, Elissa, Huang, Zhengping, Bainter, Wayne, Alosaimi, Mohammed F., Stafstrom, Kelsey, Platt, Craig D., Stauber, Tali, Raz, Somech, Tirosh, Irit, Weiss, Aaron, Jordan, Michael B., Krupski, Christa, Eleftheriou, Despina, Brogan, Paul, Sobh, Ali, Baz, Zeina, Lefranc, Gerard, Irani, Carla, Kilic, Sara S., El-Owaidy, Rasha, Lokeshwar, M.R., Pimpale, Pallavi, Khubchandani, Raju, Chambers, Eugene P., Chou, Janet, Geha, Raif S., Nigrovic, Peter A., and Zhou, Qing

Published
2020
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24. Clinical, immunological features, treatments, and outcomes of autoimmune hemolytic anemia in patients with RAG deficiency

Author

Wang, Chen, primary, Sun, Bijun, additional, Wu, Kevin, additional, Farmer, Jocelyn R., additional, Ujhazi, Boglarka, additional, Geier, Christoph B., additional, Gordon, Sumai, additional, Westermann-Clark, Emma, additional, Savic, Sinisa, additional, Secord, Elizabeth, additional, Sargur, Ravishankar, additional, Chen, Karin, additional, Jin, Jay J., additional, Dutmer, Cullen M., additional, Kanariou, Maria G., additional, Adeli, Mehdi, additional, Palma, Paolo, additional, Bonfim, Carmem, additional, Lycopoulou, Evangelia, additional, Wolska-Kusnierz, Beata, additional, Dbaibo, Ghassan, additional, Bleesing, Jack, additional, Moshous, Despina, additional, Neven, Benedicte, additional, Schuetz, Catharina, additional, Geha, Raif S., additional, Notarangelo, Luigi D., additional, Miano, Maurizio, additional, Buchbinder, David K., additional, Csomos, Krisztian, additional, Wang, Wenjie, additional, Wang, Ji-Yang, additional, Wang, Xiaochuan, additional, and Walter, Jolan E., additional

Published
2024
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25. Staphylococcus aureus Exploits Epidermal Barrier Defects in Atopic Dermatitis to Trigger Cytokine Expression

Author

Nakatsuji, Teruaki, Chen, Tiffany H, Two, Aimee M, Chun, Kimberly A, Narala, Saisindhu, Geha, Raif S, Hata, Tissa R, and Gallo, Richard L

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Emerging Infectious Diseases, Eczema / Atopic Dermatitis, 2.1 Biological and endogenous factors, Aetiology, Skin, Animals, Antibodies, Bacterial, Cells, Cultured, Cytokines, DNA, Dermatitis, Atopic, Epidermis, Filaggrin Proteins, Gene Expression Regulation, Humans, Male, Mice, Mice, Knockout, Signal Transduction, Staphylococcus aureus, Oncology and Carcinogenesis, Dermatology & Venereal Diseases, Clinical sciences
Abstract

Patients with atopic dermatitis (AD) have an abnormal skin barrier and are frequently colonized by S. aureus. In this study we investigated if S. aureus penetrates the epidermal barrier of subjects with AD and sought to understand the mechanism and functional significance of this entry. S. aureus was observed to be more abundant in the dermis of lesional skin from AD patients. Bacterial entry past the epidermis was observed in cultured human skin equivalents and in mice but was found to be increased in the skin of cathelicidin knockout and ovalbumin-sensitized filaggrin mutant mice. S. aureus penetration through the epidermis was dependent on bacterial viability and protease activity, because killed bacteria and a protease-null mutant strain of S. aureus were unable to penetrate. Entry of S. aureus directly correlated with increased expression of IL-4, IL-13, IL-22, thymic stromal lymphopoietin, and other cytokines associated with AD and with decreased expression of cathelicidin. These data illustrate how abnormalities of the epidermal barrier in AD can alter the balance of S. aureus entry into the dermis and provide an explanation for how such dermal dysbiosis results in increased inflammatory cytokines and exacerbation of disease.

Published
2016

26. Targeted deep sequencing identifies rare loss-of-function variants in IFNGR1 for risk of atopic dermatitis complicated by eczema herpeticum

Author

Gao, Li, Bin, Lianghua, Rafaels, Nicholas M, Huang, Lili, Potee, Joseph, Ruczinski, Ingo, Beaty, Terri H, Paller, Amy S, Schneider, Lynda C, Gallo, Rich, Hanifin, Jon M, Beck, Lisa A, Geha, Raif S, Mathias, Rasika A, Barnes, Kathleen C, and Leung, Donald YM

Subjects
Human Genome, Genetic Testing, Prevention, Genetics, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Adolescent, Adult, Aged, Aged, 80 and over, Cell Line, Child, Child, Preschool, Dermatitis, Atopic, Female, Genes, Reporter, Genetic Predisposition to Disease, Genotype, High-Throughput Nucleotide Sequencing, Humans, Infant, Interferon-gamma, Kaposi Varicelliform Eruption, Male, Middle Aged, Polymorphism, Single Nucleotide, Receptors, Interferon, Risk, STAT1 Transcription Factor, Young Adult, IFNGR1, genetic variants, atopic dermatitis, eczema herpeticum, Immunology, Allergy
Abstract

BackgroundA subset of atopic dermatitis is associated with increased susceptibility to eczema herpeticum (ADEH+). We previously reported that common single nucleotide polymorphisms (SNPs) in the IFN-γ (IFNG) and IFN-γ receptor 1 (IFNGR1) genes were associated with the ADEH+ phenotype.ObjectiveWe sought to interrogate the role of rare variants in interferon pathway genes for the risk of ADEH+.MethodsWe performed targeted sequencing of interferon pathway genes (IFNG, IFNGR1, IFNAR1, and IL12RB1) in 228 European American patients with AD selected according to their eczema herpeticum status, and severity was measured by using the Eczema Area and Severity Index. Replication genotyping was performed in independent samples of 219 European American and 333 African American subjects. Functional investigation of loss-of-function variants was conducted by using site-directed mutagenesis.ResultsWe identified 494 single nucleotide variants encompassing 105 kb of sequence, including 145 common, 349 (70.6%) rare (minor allele frequency

Published
2015

27. Immune dysregulation caused by homozygous mutations in CBL

Author

Janssen, Erin, Peters, Zachary, Alosaimi, Mohammed F., Smith, Emma, Milin, Elena, Stafstrom, Kelsey, Wallace, Jacqueline G., Platt, Craig D., Chou, Janet, Ansari, Yasmeen S. El, Farsi, Tariq Al, Ameziane, Najim, Al-Ali, Ruslan, Calvo, Maria, Rocha, Maria Eugenia, Bauer, Peter, Al-Sannaa, Nouriya Abbas, Sukaiti, Nashat Faud Al, Alangari, Abdullah A., Bertoli-Avella, Aida M., and Geha, Raif S.

Subjects
Gene mutations -- Physiological aspects -- Health aspects, Ubiquitin-proteasome system -- Genetic aspects, T cells -- Genetic aspects -- Health aspects, Immunologic diseases -- Genetic aspects -- Causes of, Health care industry
Abstract

CBL-B is an E3 ubiquitin ligase that ubiquitinates proteins downstream of immune receptors to downregulate positive signaling cascades. Distinct homozygous mutations in CBLB were identified in 3 unrelated children with early-onset autoimmunity, one of whom also had chronic urticaria. Patient T cells exhibited hyperproliferation in response to anti- CD3 cross-linking. One of the mutations, p.R496X, abolished CBL-B expression, and a second mutation, p.C464W, resulted in preserved CBL-B expression. The third mutation, p.H285L in the SH2 domain of CBL-B, was expressed at half the normal level in the patient's cells. Mice homozygous for the CBL-B p.H257L mutation, which corresponds to the patient's p.H285L mutation, had T and B cell hyperproliferation in response to antigen receptor cross-linking. [Cblb.sup.H257L] mice had increased percentages of T regulatory cells (Tregs) that had normal in vitro suppressive function. However, T effector cells from the patient with the p.H285L mutation and [Cblb.sup.H257L] mice were resistant to suppression by WT Tregs. Bone marrow- derived mast cells from [Cblb.sup.H257L] mice were hyperactivated after Fc[epsilon]RI cross-linking, and [Cblb.sup.H257L] mice demonstrated exaggerated IgE-mediated passive anaphylaxis. This study establishes CBL-B deficiency as a cause of immune dysregulation., Introduction The E3 ubiquitin ligase CBL-B is an important regulatory protein highly expressed in immune cells. CBL-B facilitates ubiquitination of receptor-activated signaling proteins, expediting their degradation, and plays an important [...]

Published
2022
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28. Inherited human IFN-[gamma] deficiency underlies mycobacterial disease

Author

Kerner, Gaspard, Rosain, Jeremie, Guerin, Antoine, Al-Khabaz, Ahmad, Oleaga-Quintas, Carmen, Rapaport, Franck, Massaad, Michel J., Ding, Jing-Ya, Khan, Taushif, Ali, Fatima Al, Rahman, Mahbuba, Deswarte, Caroline, Martinez-Barricarte, Ruben, Geha, Raif S., Jeanne-Julien, Valentine, Garcia, Diane, Chi, Chih-Yu, Yang, Rui, Roynard, Manon, Fleckenstein, Bernhard, Rozenberg, Flore, Boisson-Dupuis, Stephanie, Ku, Cheng-Lung, Seeleuthner, Yoann, Beziat, Vivien, Marr, Nico, Abel, Laurent, Herz, Waleed Al-, Casanova, Jean-Laurent, and Bustamante, Jacinta

Subjects
France. National Research Agency, Bacterial infections -- Development and progression -- Genetic aspects, Vaccines, BCG -- Genetic aspects, Cytokines -- Genetic aspects, B cells -- Genetic aspects, Disease susceptibility -- Genetic aspects -- Development and progression, Gene mutation -- Genetic aspects, T cells -- Genetic aspects, Codons -- Genetic aspects, Health care industry
Abstract

Mendelian susceptibility to mycobacterial disease (MSMD) is characterized by a selective predisposition to clinical disease caused by the Bacille Calmette-Guerin (BCG) vaccine and environmental mycobacteria. The known genetic etiologies of MSMD are inborn errors of IFN-[gamma] immunity due to mutations of 15 genes controlling the production of or response to IFN-[gamma]. Since the first MSMD-causing mutations were reported in 1996, biallelic mutations in the genes encoding IFN-[gamma] receptor 1 (IFN-[gamma]R1) and IFN-[gamma]R2 have been reported in many patients of diverse ancestries. Surprisingly, mutations of the gene encoding the IFN-[gamma] cytokine itself have not been reported, raising the remote possibility that there might be other agonists of the IFN-[gamma] receptor. We describe 2 Lebanese cousins with MSMD, living in Kuwait, who are both homozygous for a small deletion within the IFNG gene (c.354_357del), causing a frameshift that generates a premature stop codon (p.T119Ifs4*). The mutant allele is loss of expression and loss of function. We also show that the patients' herpesvirus Saimiri-immortalized T lymphocytes did not produce IFN-[gamma], a phenotype that can be rescued by retrotransduction with WT IFNG cDNA. The blood T and NK lymphocytes from these patients also failed to produce and secrete detectable amounts of IFN-[gamma]. Finally, we show that human IFNG has evolved under stronger negative selection than IFNGR1 or IFNGR2, suggesting that it is less tolerant to heterozygous deleterious mutations than IFNGR1 or IFNGR2. This may account for the rarity of patients with autosomal-recessive, complete IFN-[gamma] deficiency relative to patients with complete IFN-[gamma]R1 and IFN- [gamma]R2 deficiencies., Introduction Mendelian susceptibility to mycobacterial disease (MSMD) (OMIM #209950) is characterized by a predisposition to severe disease caused by weakly virulent mycobacteria, including Mycobacterium bovis Bacille Calmette-Guerin (BCG) vaccines and [...]

Published
2020
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30. Immunodeficiency and EBV-induced lymphoproliferation caused by 4-1BB deficiency

Author

Alosaimi, Mohammed F., Hoenig, Manfred, Jaber, Faris, Platt, Craig D., Jones, Jennifer, Wallace, Jacqueline, Debatin, Klaus-Michael, Schulz, Ansgar, Jacobsen, Eva, Möller, Peter, Shamseldin, Hanan E., Abdulwahab, Ferdous, Ibrahim, Niema, Alardati, Hosam, Almuhizi, Faisal, Abosoudah, Ibraheem F., Basha, Talal A., Chou, Janet, Alkuraya, Fowzan S., and Geha, Raif S.

Published
2019
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31. Injury, dysbiosis, and filaggrin deficiency drive skin inflammation through keratinocyte IL-1α release

Author

Archer, Nathan K., Jo, Jay-Hyun, Lee, Steven K., Kim, Dongwon, Smith, Barbara, Ortines, Roger V., Wang, Yu, Marchitto, Mark C., Ravipati, Advaitaa, Cai, Shuting S., Dillen, Carly A., Liu, Haiyun, Miller, Robert J., Ashbaugh, Alyssa G., Uppal, Angad S., Oyoshi, Michiko K., Malhotra, Nidhi, Hoff, Sabine, Garza, Luis A., Kong, Heidi H., Segre, Julia A., Geha, Raif S., and Miller, Lloyd S.

Published
2019
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32. Hematopoietic Stem Cell Transplantation as Treatment for Patients with DOCK8 Deficiency

Author

Aydin, Susanne E., Freeman, Alexandra F., Al-Herz, Waleed, Al-Mousa, Hamoud A., Arnaout, Rand K., Aydin, Roland C., Barlogis, Vincent, Belohradsky, Bernd H., Bonfim, Carmem, Bredius, Robbert G., Chu, Julia I., Ciocarlie, Oana C., Doğu, Figen, Gaspar, Hubert B., Geha, Raif S., Gennery, Andrew R., Hauck, Fabian, Hawwari, Abbas, Hickstein, Dennis D., Hoenig, Manfred, Ikinciogullari, Aydan, Klein, Christoph, Kumar, Ashish, Ifversen, Marianne R.S., Matthes, Susanne, Metin, Ayse, Neven, Benedicte, Pai, Sung-Yun, Parikh, Suhag H., Picard, Capucine, Renner, Ellen D., Sanal, Özden, Schulz, Ansgar S., Schuster, Friedhelm, Shah, Nirali N., Shereck, Evan B., Slatter, Mary A., Su, Helen C., van Montfrans, Joris, Woessmann, Wilhelm, Ziegler, John B., and Albert, Michael H.

Published
2019
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33. Report from the National Institute of Allergy and Infectious Diseases workshop on “Atopic dermatitis and the atopic march: Mechanisms and interventions”

Author

Davidson, Wendy F., Leung, Donald Y.M., Beck, Lisa A., Berin, Cecilia M., Boguniewicz, Mark, Busse, William W., Chatila, Talal A., Geha, Raif S., Gern, James E., Guttman-Yassky, Emma, Irvine, Alan D., Kim, Brian S., Kong, Heidi H., Lack, Gideon, Nadeau, Kari C., Schwaninger, Julie, Simpson, Angela, Simpson, Eric L., Spergel, Jonathan M., Togias, Alkis, Wahn, Ulrich, Wood, Robert A., Woodfolk, Judith A., Ziegler, Steven F., and Plaut, Marshall

Published
2019
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35. A systematic analysis of recombination activity and genotype-phenotype correlation in human recombination-activating gene 1 deficiency

Author

Lee, Yu Nee, Frugoni, Francesco, Dobbs, Kerry, Walter, Jolan E, Giliani, Silvia, Gennery, Andrew R, Al-Herz, Waleed, Haddad, Elie, LeDeist, Francoise, Bleesing, Jack H, Henderson, Lauren A, Pai, Sung-Yun, Nelson, Robert P, El-Ghoneimy, Dalia H, El-Feky, Reem A, Reda, Shereen M, Hossny, Elham, Soler-Palacin, Pere, Fuleihan, Ramsay L, Patel, Niraj C, Massaad, Michel J, Geha, Raif S, Puck, Jennifer M, Palma, Paolo, Cancrini, Caterina, Chen, Karin, Vihinen, Mauno, Alt, Frederick W, and Notarangelo, Luigi D

Subjects
Biomedical and Clinical Sciences, Immunology, Genetics, Rare Diseases, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Alleles, B-Lymphocytes, Child, Child, Preschool, Gene Order, Gene Rearrangement, Genetic Association Studies, Homeodomain Proteins, Humans, Immunoglobulin Heavy Chains, Infant, Infant, Newborn, Mutation, Phenotype, Severe Combined Immunodeficiency, T-Lymphocytes, V(D)J Recombination, Recombination-activating gene 1, V(D)J recombination, severe combined immune deficiency, Omenn syndrome, autoimmunity, genotype-phenotype correlation, immune repertoire, Allergy
Abstract

BackgroundThe recombination-activating gene (RAG) 1/2 proteins play a critical role in the development of T and B cells by initiating the VDJ recombination process that leads to generation of a broad T-cell receptor (TCR) and B-cell receptor repertoire. Pathogenic mutations in the RAG1/2 genes result in various forms of primary immunodeficiency, ranging from T(-)B(-) severe combined immune deficiency to delayed-onset disease with granuloma formation, autoimmunity, or both. It is not clear what contributes to such heterogeneity of phenotypes.ObjectiveWe sought to investigate the molecular basis for phenotypic diversity presented in patients with various RAG1 mutations.MethodsWe have developed a flow cytometry-based assay that allows analysis of RAG recombination activity based on green fluorescent protein expression and have assessed the induction of the Ighc locus rearrangements in mouse Rag1(-/-) pro-B cells reconstituted with wild-type or mutant human RAG1 (hRAG1) using deep sequencing technology.ResultsHere we demonstrate correlation between defective recombination activity of hRAG1 mutant proteins and severity of the clinical and immunologic phenotype and provide insights on the molecular mechanisms accounting for such phenotypic diversity.ConclusionsUsing a sensitive assay to measure the RAG1 activity level of 79 mutations in a physiologic setting, we demonstrate correlation between recombination activity of RAG1 mutants and the severity of clinical presentation and show that RAG1 mutants can induce specific abnormalities of the VDJ recombination process.

Published
2014

36. IL-4 receptor alpha blockade dampens allergic inflammation and upregulates IL-17A expression to promote S aureus clearance in antigen sensitized mouse skin

Author

Leyva-Castillo, Juan-Manuel, primary, McGurk, Alex, additional, Strakosha, Maria, additional, Vega-Mendoza, Daniela, additional, Smith, Sophia E.M., additional, Stafstrom, Kelsey, additional, Elkins, Megan, additional, Chou, Janet, additional, Wang, Yui-Hsi, additional, and Geha, Raif S., additional

Published
2023
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39. Author Correction: DOCK8 functions as an adaptor that links TLR-MyD88 signaling to B cell activation

Author

Jabara, Haifa H., McDonald, Douglas R., Janssen, Erin, Massaad, Michel J., Ramesh, Narayanaswamy, Borzutzky, Arturo, Rauter, Ingrid, Benson, Halli, Schneider, Lynda, Baxi, Sachin, Recher, Mike, Notarangelo, Luigi D., Wakim, Rima, Dbaibo, Ghassan, Dasouki, Majed, Al-Herz, Waleed, Barlan, Isil, Baris, Safa, Kutukculer, Necil, Ochs, Hans D., Plebani, Alessandro, Kanariou, Maria, Lefranc, Gerard, Reisli, Ismail, Fitzgerald, Katherine A., Golenbock, Douglas, Manis, John, Keles, Sevgi, Ceja, Reuben, Chatila, Talal A., and Geha, Raif S.

Published
2022
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41. A Phenotypic Approach for IUIS PID Classification and Diagnosis: Guidelines for Clinicians at the Bedside

Author

Bousfiha, Ahmed Aziz, Jeddane, Leïla, Ailal, Fatima, Al Herz, Waleed, Conley, Mary Ellen, Cunningham-Rundles, Charlotte, Etzioni, Amos, Fischer, Alain, Franco, Jose Luis, Geha, Raif S, Hammarström, Lennart, Nonoyama, Shigeaki, Ochs, Hans D, Roifman, Chaim M, Seger, Reinhard, Tang, Mimi LK, Puck, Jennifer M, Chapel, Helen, Notarangelo, Luigi D, and Casanova, Jean-Laurent

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Pediatric, Clinical Research, Algorithms, Diagnosis, Differential, Diagnostic Tests, Routine, Genotype, Humans, Immunologic Deficiency Syndromes, Immunologic Tests, Phenotype, Practice Guidelines as Topic, Primary immunodeficiency, classification, IUIS, diagnosis tool, Immunology
Abstract

The number of genetically defined Primary Immunodeficiency Diseases (PID) has increased exponentially, especially in the past decade. The biennial classification published by the IUIS PID expert committee is therefore quickly expanding, providing valuable information regarding the disease-causing genotypes, the immunological anomalies, and the associated clinical features of PIDs. These are grouped in eight, somewhat overlapping, categories of immune dysfunction. However, based on this immunological classification, the diagnosis of a specific PID from the clinician's observation of an individual clinical and/or immunological phenotype remains difficult, especially for non-PID specialists. The purpose of this work is to suggest a phenotypic classification that forms the basis for diagnostic trees, leading the physician to particular groups of PIDs, starting from clinical features and combining routine immunological investigations along the way. We present 8 colored diagnostic figures that correspond to the 8 PID groups in the IUIS Classification, including all the PIDs cited in the 2011 update of the IUIS classification and most of those reported since.

Published
2013

42. Primary Immunodeficiency Diseases: An Update on the Classification from the International Union of Immunological Societies Expert Committee for Primary Immunodeficiency

Author

Al-Herz, Waleed, Bousfiha, Aziz, Casanova, Jean-Laurent, Chapel, Helen, Conley, Mary Ellen, Cunningham-Rundles, Charlotte, Etzioni, Amos, Fischer, Alain, Franco, Jose Luis, Geha, Raif S, Hammarström, Lennart, Nonoyama, Shigeaki, Notarangelo, Luigi Daniele, Ochs, Hans Dieter, Puck, Jennifer M, Roifman, Chaim M, Seger, Reinhard, and Tang, Mimi LK

Subjects
Biomedical and Clinical Sciences, Immunology, Rare Diseases, Good Health and Well Being, primary immunodeficiency diseases, Medical Microbiology, Biochemistry and cell biology, Genetics
Abstract

We report the updated classification of primary immunodeficiency diseases, compiled by the ad hoc Expert Committee of the International Union of Immunological Societies. As compared to the previous edition, more than 15 novel disease entities have been added in the updated version. For each disorders, the key clinical and laboratory features are provided. This updated classification is meant to help in the diagnostic approach to patients with these diseases.

Published
2011

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