Targeted pharmacologic immunomodulation for inborn errors of immunity

Sacco, Keith; Stack, Michael; Notarangelo, Luigi D.

doi:10.1111/bcp.14509

Cited by 3 publications

(6 citation statements)

References 88 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This is especially true for PIDs associated with Gain-of-Function pathways [ 14 ] that can be targeted by pharmacological inhibitors, which could be already available as developed to cure cancers [ 15 ]. The early detection of such “druggable” disorders is crucial to prevent the development of severe organ damage [ 16 ].…”

Section: Introductionmentioning

confidence: 99%

Immunity and Genetics at the Revolving Doors of Diagnostics in Primary Immunodeficiencies

et al. 2021

View full text Add to dashboard Cite

Primary immunodeficiencies (PIDs) are a large and growing group of disorders commonly associated with recurrent infections. However, nowadays, we know that PIDs often carry with them consequences related to organ or hematologic autoimmunity, autoinflammation, and lymphoproliferation in addition to simple susceptibility to pathogens. Alongside this conceptual development, there has been technical advancement, given by the new but already established diagnostic possibilities offered by new genetic testing (e.g., next-generation sequencing). Nevertheless, there is also the need to understand the large number of gene variants detected with these powerful methods. That means advancing beyond genetic results and resorting to the clinical phenotype and to immunological or alternative molecular tests that allow us to prove the causative role of a genetic variant of uncertain significance and/or better define the underlying pathophysiological mechanism. Furthermore, because of the rapid availability of results, laboratory immunoassays are still critical to diagnosing many PIDs, even in screening settings. Fundamental is the integration between different specialties and the development of multidisciplinary and flexible diagnostic workflows. This paper aims to tell these evolving aspects of immunodeficiencies, which are summarized in five key messages, through introducing and exemplifying five clinical cases, focusing on diseases that could benefit targeted therapy.

show abstract

Section: Introductionmentioning

confidence: 99%

Immunity and Genetics at the Revolving Doors of Diagnostics in Primary Immunodeficiencies

et al. 2021

View full text Add to dashboard Cite

show abstract

“…This shows how seemingly unrelated conditions seem to benefit from novel therapies. The mTor pathway with the use of rapamycin has also been a successful approach for rare types of immune disorders 8 …”

mentioning

confidence: 99%

“…The 2019 classification of Inborn Errors of Immunity by the International Union of Immunological Societies Expert Committee lists 430 inborn errors of immunity 7 . In their paper for this special issue, Sacco et al 8 discuss that while many of these patients are treated symptomatically with immunoglobulins, antimicrobials or immunosuppressants, these therapies do appear to modify the underlying disease and thus subsequent morbidity or mortality and may even affect the natural history of these disorders. Some promising results have been achieved with use of haematopoietic stem cell transplantation and gene therapy which offer potential therapeutic options in this wide spectrum of immune conditions.…”

mentioning

confidence: 99%

“…In their review, Grech et al 12 describe how patients are finding hope through novel therapies such as haematopoietic stem‐cell transplantation, gene therapy, gene editing and base editing to address the underlying pathophysiology associated with this condition, which primarily include ineffective erythropoiesis, iron overload and globin chain imbalance. Interestingly jakinibs (also discussed by Sacco et al 8 ) were found to improve ineffective erythropoiesis and reversed splenomegaly in animal models of beta‐thalassaemia, however this did not translate into success in the subsequent human studies. Drugs that target transforming growth factor β (TGF‐β), such as luspatercept (ACE‐536), were also found improve erythroid maturation and red cell production and are now in clinical trial phase 13 …”

mentioning

confidence: 99%

“…Unfortunately for most patients with rare diseases, treatment does not lead to a cure and the disease burden remains lifelong. However, the understanding of the dysregulation of a specific pathway can be extremely useful both prognostically and therapeutically 8 . Such mechanistic studies can lead to better and more robust models of disease and, eventually, successful approaches to treatment at a clinical level.…”

mentioning

confidence: 99%

See 2 more Smart Citations

Addressing the challenges of novel therapies in rare diseases with mechanistic perspectives: Missed opportunities or the way forward?

Mifsud

Cranswick

2022

Brit J Clinical Pharma

View full text Add to dashboard Cite

There is no universally agreed definition of what is a rare disease.Depending upon the jurisdiction, the incidence of rare is defined as occurring in less than one in 1500 (in the United States) to one in 2000 (European Union). Rare Diseases Day falls on the 29 February but often celebrated on 28 February during a non-leap year. While individually such conditions are clearly uncommon, with approximately 8000 rare diseases identified, they cumulatively encompass a significant portion of the population. It is estimated that, worldwide, there are 400 million people living with a rare disease. Rare diseases have, in the past, been largely neglected by the pharmaceutical industry who calculated that the development of a therapy for an uncommon indication was unlikely to be profitable. This lacuna was recognised by governments internationally with the enactment of the Orphan Drug Act in the United States in 1983, and the EU orphan drug designation 2000. This led to huge impetus towards the discovery of new therapies for rare diseases. 1 This special issue of the British Journal of Clinical Pharmacology Reviews, in fact, attempts to address the knowledge gained in the last few decades on novel perspectives and mechanism in the search for new potential treatments for rare diseases. The issue includes six papers encompassing a variety of rare diseases where the authors have used varying perspectives in the identification of innovative tools in this quest.Various stakeholders have become motivated (for various and not always altruistic reasons) to search for new therapies for these conditions as described in Kesselheim and Solomon 2 in their discussion of the use of colchicine for some rare diseases. Yet the path is far from smooth. The initial monetary outlay needed, with huge attrition rates of what seem to be promising lead compounds, have led to big pharma seeking to think out of the box and turn to novel mechanistic perspectives to identify new opportunities for those rare conditions which previously were considered to be without hope. 3 As Forbes et al. 4 describe in their review for this special issue, the scarcity of disease-modifying therapies for rare diseases is a challenge, not only due to a lack of understanding of the underlying molecular disease mechanisms, but also the difficulties in recruiting the number of patients which will ensure that clinical trials of these drugs are sufficiently powered to pass regulatory hurdles.

show abstract

Difetti congeniti dell’immunità: non solo le vecchie immunodeficienze

Tommasini,

Valencic,

Naviglio

2024

Medico E Bambino

View full text Add to dashboard Cite

Inborn errors of immunity are a rapidly-developing area of clinical study. Based on the description of a small set of disorders with a significant risk of infection that may be identified with a small number of lab tests, the definition has been expanded to include a broader range of diseases that may necessitate a more intricate diagnostic process involving immunological and genetic studies. In this context, the paper presents a compilation of the most prevalent and severe illnesses that should not be overlooked. Additionally, it provides valuable guidance for classifying recently identified conditions, which may manifest as more nuanced and gradual clinical presentations. Prompt identification is es- sential for timely implementation of elective treatments such as bone marrow transplantation or gene therapy in severe instances or for commencing targeted medications that can mitigate present and future hazards in other cases.

show abstract

Targeted pharmacologic immunomodulation for inborn errors of immunity

Cited by 3 publications

References 88 publications

Immunity and Genetics at the Revolving Doors of Diagnostics in Primary Immunodeficiencies

Immunity and Genetics at the Revolving Doors of Diagnostics in Primary Immunodeficiencies

Addressing the challenges of novel therapies in rare diseases with mechanistic perspectives: Missed opportunities or the way forward?

Difetti congeniti dell’immunità: non solo le vecchie immunodeficienze

Contact Info

Product

Resources

About