Thymus and aging: morphological, radiological, and functional overview

Rezzani, Rita; Nardo, Lorenzo; Favero, Gaia; Peroni, Michele; Rodella, Luigi Fabrizio

doi:10.1007/s11357-013-9564-5

Cited by 146 publications

(111 citation statements)

References 219 publications

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“…By 50 y of age around 80% of functional thymus tissue has been lost. 10 Our model predicts that the hepatitis B seroprotection rate remains 90% up to 49 y of age, and above 80% until 60 y of age in adults who are otherwise healthy. While we did not investigate interactions between gender and immune senescence, our results are comparable to results of a modeling study of anti-HBs concentrations in more than 11,000 healthy adults in the Netherlands.…”

Section: Introductionmentioning

confidence: 87%

“…[5][6][7][8][9] Immune senescence is characterized by altered composition of bone marrow with reduced capacity to produce and nurture stem cells, and atrophy of the thymus gland with reduced output of Tcells. 10 The response to vaccination is impaired in the elderly due to functional defects at multiple levels in innate and adaptive immune responses. These include reduced capacity of antigen presenting cells to take up and present antigen, lower numbers of T-cells capable of responding to new antigen, reduced magnitude and quantity of the B-cell antibody response, and poor effector T-cell activation and signaling due to reduced numbers and loss of receptor diversity.…”

Section: Introductionmentioning

confidence: 99%

“…10,29 Thymic involution is one of the most important events that contributes to immune dysfunction in the elderly. 10,29 Evidence of early and continual decreases in vaccine responses with age is broadly consistent with the process of thymic involution, which begins in early adulthood. By 50 y of age around 80% of functional thymus tissue has been lost.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Characterization of an age-response relationship to GSK's recombinant hepatitis B vaccine in healthy adults: An integrated analysis

Meeren¹,

Crasta²,

Cheuvart³

et al. 2015

Human Vaccines & Immunotherapeutics

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The immune system becomes less effective with age, and older age is associated with an increased susceptibility to diseases and reduced responses to vaccination. Furthermore, some adult populations, such as those with diabetes mellitus, are at increased risk of acute hepatitis B virus (HBV) infection. Decreasing responses to vaccination with advanced age have been described, but it is not known at what age immunogenicity starts to reduce, or until what age immunogenicity remains acceptable (for example 80 % seroprotection post-vaccination). We characterized the relationship between age and seroprotection rate induced by recombinant HBV vaccination by conducting a pooled analysis of clinical trial data. Healthy adults aged 20 y who had been vaccinated with 20mg HBV vaccine (Engerix TM B, GSK Vaccines, Belgium) in a 0, 1, 6 months schedule in 11 studies since 1996 were included. The observed seroprotection rate, defined as an anti-HBV surface antigen antibody concentration 10 mIU/ml was 94.5% in the whole population (N D 2,620, Total vaccinated cohort), ranging from 98.6% in adults vaccinated at age 20-24 years, to 64.8% in those vaccinated at age 65 y A model on seroprotection rates showed a statistically significant decrease with age, and predicted that the anti-HBs seroprotection rate remains 90% up to 49 y of age and 80% up to 60 y of age. Individuals at risk of HBV infection should be vaccinated as early in life as possible to improve the likelihood of achieving seroprotection. Additional studies are needed to identify whether unvaccinated individuals older than 60 y would benefit from regimens that include additional or higher vaccine doses.

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Section: Introductionmentioning

confidence: 87%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Characterization of an age-response relationship to GSK's recombinant hepatitis B vaccine in healthy adults: An integrated analysis

Meeren¹,

Crasta²,

Cheuvart³

et al. 2015

Human Vaccines & Immunotherapeutics

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show abstract

“…Postnatal. At birth the thymus is fully formed morphologically, its size relative to body size is at its peak and it has maximal thymocyte output at early postnatal life [41,42]. This may be followed by a temporary decrease until late infancy, with continuous growth thereafter until involution (including replacement of thymus parenchyma by adipose tissue) in adolescence (reviewed by [42]).…”

Section: Yolk Sac Liver Bone Marrow Spleen Thymusmentioning

confidence: 99%

Development of immune organs and functioning in humans and test animals: Implications for immune intervention studies

Kuper¹,

Bilsen²,

Cnossen³

et al. 2016

Reproductive Toxicology

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“…Aged humans develop a variety of autoantibodies, and display poor response to vaccines and increased susceptibility to both viral and bacterial infections. The progressive impairment in immune functions include progressive T cell deficiency, which is contributed by thymic involution [1], increased apoptosis of T cells and T cell subsets [2][3][4], and impaired priming of T cells by DCs [5][6][7]; B cell dysfunctions are revealed by impaired specific antibody response to vaccines, and development of autoimmunity [8][9][10][11][12].…”

Section: Introductionmentioning

confidence: 99%

Role of Dendritic Cells in Autoimmunity in Aged Humans

Gupta¹

2014

Immunome Res

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Immunological tolerance to self-antigen is mediated by deletion of self-reactive lymphocytes by apoptosis, unresponsiveness to self-antigens (anergy), regulation by T cells (Treg), and efficient removal of apoptotic bodies by phagocytic cells. Dendritic cells (DCs) play an important role in both tolerance (predominantly via induction of Treg) and inthe induction of immune response to non-self antigens. Therefore, an impairment of DCs functions may result in the loss of tolerance and induction of immune response to self-antigens, resulting in autoimmunity. Aging represents a paradox of impaired response to non-self antigens, and an increased response to self-antigens, resulting in an increased susceptibility to infections, and development of autoimmunity in aged humans. I have reviewed the role of DCs and mechanisms involved in autoimmunity, including epigenetic changes in aged DNA, and histone modifications in chromatin in human aging.

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Thymus and aging: morphological, radiological, and functional overview

Cited by 146 publications

References 219 publications

Characterization of an age-response relationship to GSK's recombinant hepatitis B vaccine in healthy adults: An integrated analysis

Characterization of an age-response relationship to GSK's recombinant hepatitis B vaccine in healthy adults: An integrated analysis

Development of immune organs and functioning in humans and test animals: Implications for immune intervention studies

Role of Dendritic Cells in Autoimmunity in Aged Humans

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