Literature DB >> 31737589

Hematopoietic Stem Cell Transplantation for Primary Immunodeficiencies.

Andrew R Gennery^1,2, Michael H Albert³, Mary A Slatter^1,2, Arjan Lankester⁴.

Abstract

The field of primary immunodeficiencies has pioneered many of the advances in haematopoietic stem cell transplantation and cellular therapies over the last 50 years. The first patients to demonstrate sustained benefit and prolonged cure from the primary genetic defect following allogeneic haematopoietic stem cell transplantation were patients with primary immunodeficiencies. Although primary immunodeficiency patients began the modern era of haematopoietic stem cell transplantation, the history is nevertheless short-in answer to the question "what is the long term outcome of patients transplanted for primary immunodeficiencies?" we often have to say that we do not know. We believe that most patients who undergo haematopoietic stem cell transplantation for primary immunodeficiencies should live a normal lifespan with a fully corrected immune system. We are now beginning to understanding long term outcomes, the relationship to the underlying genetic defect, age, and pre-morbid condition of the patient at time of transplantation, stem cell source and donor, and effect of pre-transplant cytoreductive chemotherapy conditioning. The long term consequences of post-transplant complications such as graft vs. host disease, veno-occlusive disease, or immune dysregulation are also being recognized. Additionally, some genetic defects have a systemic distribution, and we are learning the natural history of these defects once the immunodeficiency has been removed.

Entities: Chemical Disease Gene Species

Keywords: Wiskott Aldrich syndrome; chronic granulomatous disease; conditioning; primary immunodeficiency; severe combined immnunodeficiency

Year: 2019 PMID： 31737589 PMCID： PMC6831554 DOI： 10.3389/fped.2019.00445

Source DB: PubMed Journal: Front Pediatr ISSN： 2296-2360 Impact factor: 3.418

The field of primary immunodeficiencies has pioneered the way in many of the advances in hematopoietic stem cell transplantation and cellular therapies over the last 50 years. In 1968, three patients with primary immunodeficiencies—one with Wiskott Aldrich syndrome and two with X-linked severe combined immunodeficiencies—were the first patients to demonstrate sustained benefit and prolonged cure from the primary genetic defect following allogeneic hematopoietic stem cell transplantation (1–3). The story of our specialty, whilst at the inception of hematopoietic stem cell transplantation, is thus short—in answer to the question “what is the long term outcome of patients transplanted for primary immunodeficiencies?,” we often have to say that we do not really know. We believe, in many cases, that patients who undergo hematopoietic stem cell transplantation for primary immunodeficiencies will live a normal lifespan with a fully corrected immune system. However, it is only now that we are beginning to dissect long term outcomes and the relationship to the underlying genetic defect, age and pre-morbid condition of the patient at time of transplantation, stem cell source and donor, and effect of pre-transplant cytoreductive chemotherapy conditioning (4–8). The long term consequences of post-transplant complications such as graft vs. host disease, veno-occlusive disease or immune dysregulation are also being recognized. Additionally, some genetic defects have a systemic distribution, and we are learning the natural history of these defects once the immunodeficiency has been removed. We are hindered by dealing with small numbers of patients, rare diseases, changing protocols and transplant techniques, as well as suboptimal methods of measuring immune function and repertoire, and incomplete follow up information. Furthermore, the information we gather in our retrospective studies often pertains to historic rather than current practice (9). Importantly, we are also, for many diseases, beginning to understand the natural history of the disease without intervention with transplantation, so that, for some of the more common diseases, we are able to compare data between transplanted and non-transplanted cohorts (10–14). Nevertheless, we are entering an era where we are beginning to understand the implications and consequences of previous treatment practice. Data that we are now gathering are important to aid our understanding of the impact of transplantation on patient survival, immune function, long term organ dysfunction/toxicity including fertility, and quality of life (refer to chapter on Long Term Outcome and Immune Function After Hematopoietic Stem Cell Transplantation for Primary Immunodeficiency). It is now clear that early transplant before the onset of significant infection or organ dysfunction results in better outcomes for all immunodeficiencies (14, 15). In recent years, this knowledge and has heralded the introduction of newborn screening to identify patients with severe combined immunodeficiency before symptom onset (16) (refer to chapter on Newborn Screening for SCID). Furthermore, data are emerging to suggest that best early and longer term outcomes of immune function require some degree of myeloid engraftment which reflects hematopoietic stem cell progenitor engraftment, and by implication, some form of pre-transplant conditioning (4, 6, 17, 18). Our understanding of the underlying genetic defects has led us to realize that the degree of donor chimerism required for optimal outcome differs depending on the primary disease—a small percentage of donor myeloid chimerism in patients with RAG-deficient severe combined immunodeficiency is sufficient to restore complete T- and B-lymphocyte repertoire and function, whereas incomplete donor chimerism in patients with Wiskott-Aldrich syndrome is associated with an increased risk of autoimmunity (7). Patients with gain-of-function diseases such as STAT-1 or APDS appear to be more likely to experience recurrence of disease manifestations when complete donor chimerism is not achieved (19, 20) (refer to chapter on Long Term Outcome and Immune Function After Hematopoietic Stem Cell Transplantation for Primary Immunodeficiency). Detailed information from larger cohorts of these patients, and those treated with small molecules or specific pathway inhibitors will help us to appropriately select patients for transplantation in the future (21). An understanding of the toxicities resulting from our treatment approaches has driven the search for safer approaches to therapy, and resulted in less toxic chemotherapy conditioning regimens (22, 23), and is leading to approaches in antibody-based conditioning regimens (24, 25) (refer to chapter on Conditioning Perspectives for Primary Immunodeficiency Stem cell Transplants) and safer approaches to curative therapy including genetic correction of autologous cells by gene addition (26) or gene editing (refer to chapter Autologous stem cell-based gene therapy for inherited disorders: state-of-the-art and future prospects). Our understanding of disease phenotype is being complicated as the genetic revolution, powered by new generation sequencing techniques and analysis of big data sets, reveals patients with new, less severe phenotypes who harbor mutations in genes previously understood to confer a severe phenotype. At the same time as transplantation becomes safer, it is also becoming clear that not everyone with a specific primary immunodeficiency will require transplantation (27). Nowhere is this dilemma sharper than in the expanding field of adolescent and young adult transplantation for primary immunodeficiency (28, 29) (refer to chapter on HSCT in Adolescents and Young Adults with Primary Immunodeficiencies). It should be acknowledged that most of our data pertain to treatment of infants or children, and cannot be automatically extrapolated to older patients. Recognizing who in this group of patients requires transplantation, or can be adequately managed with newly emerging immune-specific therapies is probably one of the most difficult current challenges. The need for collaboration between specialists, particularly through organizations like the Inborn Errors Working Party of the European Society for Blood and Marrow Transplantation (IEWP-EBMT), the Primary Immune Deficiency Treatment Consortium (PIDTC) of North America, the European Society for Immunodeficiencies (ESID), and Stem CEll Transplant for primary Immune Deficiencies in Europe (SCETIDE) and the harvesting of good quality data into specialist registries has never been greater. As we celebrate 50 years of transplantation for primary immunodeficiencies, we can acknowledge the tremendous progress that we have achieved and look to a bright future for our patients fuelled by enthusiastic international professional collaborations between clinical specialists, basic scientists, patient organizations and industry. These collaborations should now focus on specific questions, identifying current knowledge (30), and formulating practical research questions for the future (31). Given the rarity of our patients, and relatively small cohorts of patients, it is only by close collaborative efforts, ideally between relevant societies such as those listed above, and careful use of combined registries data, with carefully directed questions that we will begin to gather the answers. Retrospective data harvesting has formed the foundation of our knowledge base to date, piecing together knowledge from different studies, often measuring diverse parameters. Perhaps now, building on the knowledge we have now accumulated, is the time to design prospective clinical trials for our patients, in order to accurately answer outstanding questions.

Author Contributions

AG, MA, MS, and AL wrote and edited the manuscript.

Conflict of Interest

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

31 in total

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Authors: J De Koning; D W Van Bekkum; K A Dicke; L J Dooren; J Rádl; J J Van Rood
Journal: Lancet Date: 1969-06-21 Impact factor: 79.321

Review 2. Recommendations for Screening and Management of Late Effects in Patients with Severe Combined Immunodeficiency after Allogenic Hematopoietic Cell Transplantation: A Consensus Statement from the Second Pediatric Blood and Marrow Transplant Consortium International Conference on Late Effects after Pediatric HCT.

Authors: Jennifer Heimall; Rebecca H Buckley; Jennifer Puck; Thomas A Fleisher; Andrew R Gennery; Elie Haddad; Benedicte Neven; Mary Slatter; Skinner Roderick; K Scott Baker; Andrew C Dietz; Christine Duncan; Linda M Griffith; Luigi Notarangelo; Michael A Pulsipher; Morton J Cowan
Journal: Biol Blood Marrow Transplant Date: 2017-05-04 Impact factor: 5.742

3. SCID genotype and 6-month posttransplant CD4 count predict survival and immune recovery.

Authors: Elie Haddad; Brent R Logan; Linda M Griffith; Rebecca H Buckley; Roberta E Parrott; Susan E Prockop; Trudy N Small; Jessica Chaisson; Christopher C Dvorak; Megan Murnane; Neena Kapoor; Hisham Abdel-Azim; Imelda C Hanson; Caridad Martinez; Jack J H Bleesing; Sharat Chandra; Angela R Smith; Matthew E Cavanaugh; Soma Jyonouchi; Kathleen E Sullivan; Lauri Burroughs; Suzanne Skoda-Smith; Ann E Haight; Audrey G Tumlin; Troy C Quigg; Candace Taylor; Blachy J Dávila Saldaña; Michael D Keller; Christine M Seroogy; Kenneth B Desantes; Aleksandra Petrovic; Jennifer W Leiding; David C Shyr; Hélène Decaluwe; Pierre Teira; Alfred P Gillio; Alan P Knutsen; Theodore B Moore; Morris Kletzel; John A Craddock; Victor Aquino; Jeffrey H Davis; Lolie C Yu; Geoffrey D E Cuvelier; Jeffrey J Bednarski; Frederick D Goldman; Elizabeth M Kang; Evan Shereck; Matthew H Porteus; James A Connelly; Thomas A Fleisher; Harry L Malech; William T Shearer; Paul Szabolcs; Monica S Thakar; Mark T Vander Lugt; Jennifer Heimall; Ziyan Yin; Michael A Pulsipher; Sung-Yun Pai; Donald B Kohn; Jennifer M Puck; Morton J Cowan; Richard J O'Reilly; Luigi D Notarangelo
Journal: Blood Date: 2018-08-28 Impact factor: 22.113

4. Radioimmunotherapy-based conditioning for hematopoietic cell transplantation in children with malignant and nonmalignant diseases.

Authors: Ansgar S Schulz; Gerhard Glatting; Manfred Hoenig; Catharina Schuetz; Susanne A Gatz; Simon Grewendorf; Monika Sparber-Sauer; Rainer Muche; Norbert Blumstein; Gabriele Kropshofer; Meinolf Suttorp; Donald Bunjes; Klaus-Michael Debatin; Sven N Reske; Wilhelm Friedrich
Journal: Blood Date: 2011-02-15 Impact factor: 22.113

5. Long-term outcomes of 176 patients with X-linked hyper-IgM syndrome treated with or without hematopoietic cell transplantation.

Authors: M Teresa de la Morena; David Leonard; Troy R Torgerson; Otavio Cabral-Marques; Mary Slatter; Asghar Aghamohammadi; Sharat Chandra; Luis Murguia-Favela; Francisco A Bonilla; Maria Kanariou; Rongras Damrongwatanasuk; Caroline Y Kuo; Christopher C Dvorak; Isabelle Meyts; Karin Chen; Lisa Kobrynski; Neena Kapoor; Darko Richter; Daniela DiGiovanni; Fatima Dhalla; Evangelia Farmaki; Carsten Speckmann; Teresa Español; Anna Shcherbina; Imelda Celine Hanson; Jiri Litzman; John M Routes; Melanie Wong; Ramsay Fuleihan; Suranjith L Seneviratne; Trudy N Small; Ales Janda; Liliana Bezrodnik; Reinhard Seger; Andrea Gomez Raccio; J David M Edgar; Janet Chou; Jordan K Abbott; Joris van Montfrans; Luis Ignacio González-Granado; Nancy Bunin; Necil Kutukculer; Paul Gray; Gisela Seminario; Srdjan Pasic; Victor Aquino; Christian Wysocki; Hassan Abolhassani; Morna Dorsey; Charlotte Cunningham-Rundles; Alan P Knutsen; John Sleasman; Beatriz Tavares Costa Carvalho; Antonio Condino-Neto; Eyal Grunebaum; Helen Chapel; Hans D Ochs; Alexandra Filipovich; Mort Cowan; Andrew Gennery; Andrew Cant; Luigi D Notarangelo; Chaim M Roifman
Journal: J Allergy Clin Immunol Date: 2016-09-30 Impact factor: 10.793

6. Update on the safety and efficacy of retroviral gene therapy for immunodeficiency due to adenosine deaminase deficiency.

Authors: Maria Pia Cicalese; Francesca Ferrua; Laura Castagnaro; Roberta Pajno; Federica Barzaghi; Stefania Giannelli; Francesca Dionisio; Immacolata Brigida; Marco Bonopane; Miriam Casiraghi; Antonella Tabucchi; Filippo Carlucci; Eyal Grunebaum; Mehdi Adeli; Robbert G Bredius; Jennifer M Puck; Polina Stepensky; Ilhan Tezcan; Katie Rolfe; Erika De Boever; Rickey R Reinhardt; Jonathan Appleby; Fabio Ciceri; Maria Grazia Roncarolo; Alessandro Aiuti
Journal: Blood Date: 2016-04-29 Impact factor: 22.113

7. Treosulfan-based conditioning for allogeneic HSCT in children with chronic granulomatous disease: a multicenter experience.

Authors: Beatriz Morillo-Gutierrez; Rita Beier; Kanchan Rao; Lauri Burroughs; Ansgar Schulz; Anna-Maria Ewins; Brenda Gibson; Petr Sedlacek; Ladislav Krol; Brigitte Strahm; Irina Zaidman; Krzysztof Kalwak; Julie-An Talano; Ann Woolfrey; Chris Fraser; Isabelle Meyts; Ingo Müller; Jacek Wachowiak; Maria Ester Bernardo; Paul Veys; Karl-Walter Sykora; Andrew R Gennery; Mary Slatter
Journal: Blood Date: 2016-05-23 Impact factor: 22.113

8. Jakinibs for the treatment of immune dysregulation in patients with gain-of-function signal transducer and activator of transcription 1 (STAT1) or STAT3 mutations.

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Journal: J Allergy Clin Immunol Date: 2018-08-06 Impact factor: 10.793

9. Clinical outcome in children with chronic granulomatous disease managed conservatively or with hematopoietic stem cell transplantation.

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Journal: J Allergy Clin Immunol Date: 2013-07-16 Impact factor: 10.793

10. Long-term follow-up of IPEX syndrome patients after different therapeutic strategies: An international multicenter retrospective study.

Authors: Federica Barzaghi; Laura Cristina Amaya Hernandez; Benedicte Neven; Silvia Ricci; Zeynep Yesim Kucuk; Jack J Bleesing; Zohreh Nademi; Mary Anne Slatter; Erlinda Rose Ulloa; Anna Shcherbina; Anna Roppelt; Austen Worth; Juliana Silva; Alessandro Aiuti; Luis Murguia-Favela; Carsten Speckmann; Magda Carneiro-Sampaio; Juliana Folloni Fernandes; Safa Baris; Ahmet Ozen; Elif Karakoc-Aydiner; Ayca Kiykim; Ansgar Schulz; Sandra Steinmann; Lucia Dora Notarangelo; Eleonora Gambineri; Paolo Lionetti; William Thomas Shearer; Lisa R Forbes; Caridad Martinez; Despina Moshous; Stephane Blanche; Alain Fisher; Frank M Ruemmele; Come Tissandier; Marie Ouachee-Chardin; Frédéric Rieux-Laucat; Marina Cavazzana; Waseem Qasim; Barbarella Lucarelli; Michael H Albert; Ichiro Kobayashi; Laura Alonso; Cristina Diaz De Heredia; Hirokazu Kanegane; Anita Lawitschka; Jong Jin Seo; Marta Gonzalez-Vicent; Miguel Angel Diaz; Rakesh Kumar Goyal; Martin G Sauer; Akif Yesilipek; Minsoo Kim; Yesim Yilmaz-Demirdag; Monica Bhatia; Julie Khlevner; Erick J Richmond Padilla; Silvana Martino; Davide Montin; Olaf Neth; Agueda Molinos-Quintana; Justo Valverde-Fernandez; Arnon Broides; Vered Pinsk; Antje Ballauf; Filomeen Haerynck; Victoria Bordon; Catharina Dhooge; Maria Laura Garcia-Lloret; Robbert G Bredius; Krzysztof Kałwak; Elie Haddad; Markus Gerhard Seidel; Gregor Duckers; Sung-Yun Pai; Christopher C Dvorak; Stephan Ehl; Franco Locatelli; Frederick Goldman; Andrew Richard Gennery; Mort J Cowan; Maria-Grazia Roncarolo; Rosa Bacchetta
Journal: J Allergy Clin Immunol Date: 2017-12-11 Impact factor: 10.793

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Journal: PLoS One Date: 2021-11-03 Impact factor: 3.752

2. Tailored therapies for primary immunodeficiencies.

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Journal: Acta Biomed Date: 2021-11-29

Review 3. Update on Clinical Ex Vivo Hematopoietic Stem Cell Gene Therapy for Inherited Monogenic Diseases.

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Journal: Mol Ther Date: 2020-11-20 Impact factor: 11.454

4. Hematopoietic Cell Transplantation for Chronic Granulomatous Disease in Japan.

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Journal: Front Immunol Date: 2020-07-29 Impact factor: 7.561

4 in total