Inherited GINS1 deficiency underlies growth retardation along with neutropenia and NK cell deficiency

Cottineau, Julien; Kottemann, Molly C.; Lach, Francis P.; Kang, Young Hoon; Vély, Frederic; Deenick, Elissa K.; Lazarov, Tomi; Gineau, Laure; Wang, Yi; Farina, Andrea; Chansel, Marie; Lorenzo, Lazaro; Pipéroglou, Christelle; Cindy, S.; Nitschké, Patrick; Belkadi, Aziz; Itan, Yuval; Boisson, Bertrand; Jabot–Hanin, Fabienne; Pïcard, Capucine; Bustamante, Jacinta; Eidenschenk, Céline; Boucherit, Soraya; Aladjidi, Nathalie; Lacombe, Didier; Barat, P.; Qasim, Waseem; Hurst, Jane A.; Pollard, Andrew J.; Uhlig, Holm H.; Fieschi, Claire; Michon, Jean; Bermudez, Vladimir P.; Abel, Laurent; Villartay, Jean‐Pierre de; Geissmann, Frédéric; Tangye, Stuart G.; Hurwitz, Jerard; Vivier, Éric; Casanova, Jean Laurent; Smogorzewska, Agata; Jouanguy, Emmanuelle

doi:10.1172/jci90727

Cited by 121 publications

(173 citation statements)

References 49 publications

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“…Like the MCM4‐deficient patients, they also had some extra‐immune manifestations including short stature and dysmorphic features. Whole exome sequencing identified mutations in GINS1 , leading to decreased protein expression of GINS1 and other GINS complex members . As with MCM4 mutations, biochemical analysis demonstrated impaired initiation of DNA replication in patient fibroblasts, and cells containing damaging GINS1 variants had cell cycle arrest and induction of DNA damage repair pathways measured by γH2AX staining.…”

Section: Classical Nkd (Cnkd)mentioning

confidence: 97%

“…Given the rarity of NKD, there is an increasingly strong signal around the theme of genes associated with cell cycle and proliferation in NKD. Mutations in MCM4 and GINS1 all lead to a strikingly similar NK cell phenotype with seemingly little involvement of other lymphocyte lineages . While less well described, mutations in other DNA replication and repair enzymes also lead to NK cell aberrations, including RTEL1 , ZBTB24 , and POLE2 …”

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

“…This could account for the delayed onset, in some cases well into adulthood, of NKD that could affect the stem cell subset, particularly GATA2 deficiency. It is also important to consider the natural history of exposure to herpesviral infections as a driver of NK cell subsets and activation/maturation, particularly as many of these happen in adolescence and likely account for the timing of appearance of symptoms, particularly in patients with IRF8 and CMG helicase mutations …”

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

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Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Mace

Orange

2018

Immunological Reviews

133

107

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Human NK cells are innate immune effectors that play a critical roles in the control of viral infection and malignancy. The importance of their homeostasis and function can be demonstrated by the study of patients with primary immunodeficiencies (PID), which are part of the family of diseases known as inborn defects of immunity. While NK cells are affected in many PIDs in ways that may contribute to a patient’s clinical phenotype, a small number of PIDs have an NK cell abnormality as their major immunological defect. These PIDs can be collectively referred to as NK cell deficiency disorders (NKD), and include effects upon NK cell numbers, subsets and/or functions. The clinical impact of NKD can be severe including fatal viral infection, with particular susceptibility to herpesviral infections, such as cytomegalovirus, varicella zoster virus and Epstein-Barr virus. While NKD is rare, studies of these diseases are important for defining specific requirements for human NK cell development and homeostasis. New themes in NK cell biology are emerging through the study of both known and novel NKD, particularly those affecting cell cycle and DNA damage repair, as well as broader PIDs having substantive impact upon NK cells. In addition, the discovery of NKD that affect other innate lymphoid cell (ILC) subsets opens new doors for better understanding the relationship between conventional NK cells and other ILC subsets. Here we describe the biology underlying human NKD, particularly in the context of new insights into innate immune cell function, including a discussion of recently described NKD with accompanying effects on ILC subsets. Given the impact of these disorders upon human immunity with a common focus upon NK cells, the unifying message of a critical role for NK cells in human host defense singularly emerges.

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Section: Classical Nkd (Cnkd)mentioning

confidence: 97%

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

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Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Mace

Orange

2018

Immunological Reviews

133

107

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“…The etiology of NK cell deficiency was also linked with mutations in GINS1 , which encodes a subunit of CMG helicase [153]. More interestingly, a missense variant in MCM2 has been described to be associated with a dominant disorder characterized by progressive hearing loss [154].…”

Section: Human Genetic Diseases Associated With Origin Licensing Amentioning

confidence: 99%

Dormant origins as a built-in safeguard in eukaryotic DNA replication against genome instability and disease development

Shima

Pederson

2017

DNA Repair

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DNA replication is a prerequisite for cell proliferation, yet it can be increasingly challenging for a eukaryotic cell to faithfully duplicate its genome as its size and complexity expands. Dormant origins now emerge as a key component for cells to successfully accomplish such a demanding but essential task. In this perspective, we will first provide an overview of the fundamental processes eukaryotic cells have developed to regulate origin licensing and firing. With a special focus on mammalian systems, we will then highlight the role of dormant origins in preventing replication-associated genome instability and their functional interplay with proteins involved in the DNA damage repair response for tumor suppression. Lastly, deficiencies in the origin licensing machinery will be discussed in relation to their influence on stem cell maintenance and human diseases.

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“…Cottineau et al determined that the amount of GINS1 expressed in patientderived cells ranges from 29% to 53% of the level of GINS1 generated by cells from healthy controls (1). This reduced expression apparently leads to decreased expression of GINS3 and GINS4, resulting in defective GINS complex assembly.…”

mentioning

confidence: 99%

Defects in DNA replication hit NK cells and neutrophils

Ley¹

2017

Journal of Clinical Investigation

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Inherited GINS1 deficiency underlies growth retardation along with neutropenia and NK cell deficiency

Cited by 121 publications

References 49 publications

Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Dormant origins as a built-in safeguard in eukaryotic DNA replication against genome instability and disease development

Defects in DNA replication hit NK cells and neutrophils

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