The genetic basis of ankylosing spondylitis: new insights into disease pathogenesis

Tsui, Florence W. L.; Tsui, Hing Wo; Akram, Ali; Haroon, Nigil; Inman, Robert D.

doi:10.2147/tacg.s37325

Cited by 94 publications

(70 citation statements)

References 98 publications

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“…The presence of amino acid Asp or histidine (His) at position 116 is the only difference between B*2705 and B*2709. There are three principle features of HLA-B27 that are known to distinguish it from other HLA class I molecules such as the peptide-binding specificity, the tendency to misfold and the predilection for forming heavy chain homodimers during cell-surface recycling [177,180,182]. The current hypotheses linking HLA-B27 to spondyloarthritis pathogenesis includes (1) Arthritogenic peptides: self-peptides selected and presented by properly folded forms of HLA-B27 complexed with b2 m have been hypothesized to be the target of autoreactive CD8 + T cells and serve as an upstream initiator of inflammation, (2) recognition of non-canonical HLA-B27: naturally occurring cell-surface HLA-B27 dimers are hypothesized to be recognized by killer immunoglobulin receptors (such as KIR3DL2) in the leucocyte immunoglobulin-like receptor family (LILR) and trigger inflammation and (3) HLA-B27 misfolding: the formation of misfolded oligomers and BiP binding by newly synthesized HLA-B27 heavy chains causes ER stress, which has intrinsic effects on cellular function that are hypothesized to promote development of spondyloarthritis.…”

Section: Hla and Autoimmune Diseasesmentioning

confidence: 99%

“…The current hypotheses linking HLA-B27 to spondyloarthritis pathogenesis includes (1) Arthritogenic peptides: self-peptides selected and presented by properly folded forms of HLA-B27 complexed with b2 m have been hypothesized to be the target of autoreactive CD8 + T cells and serve as an upstream initiator of inflammation, (2) recognition of non-canonical HLA-B27: naturally occurring cell-surface HLA-B27 dimers are hypothesized to be recognized by killer immunoglobulin receptors (such as KIR3DL2) in the leucocyte immunoglobulin-like receptor family (LILR) and trigger inflammation and (3) HLA-B27 misfolding: the formation of misfolded oligomers and BiP binding by newly synthesized HLA-B27 heavy chains causes ER stress, which has intrinsic effects on cellular function that are hypothesized to promote development of spondyloarthritis. HLA-B27 can exhibit all three of these behaviours in the same cell and these concepts are not mutually exclusive [182].…”

Section: Hla and Autoimmune Diseasesmentioning

confidence: 99%

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Clinical Role of Human Leukocyte Antigen in Health and Disease

2015

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Most of the genes in the major histocompatibility complex (MHC) region express high polymorphism that is fundamental for their function. The most important function of human leukocyte antigen (HLA) molecule is in the induction, regulation of immune responses and the selection of the T cell repertoire. A clinician's attention is normally drawn to a system only when it malfunctions. The HLA system is no exception in this regard, but in contrast to other systems, it also arouses interest when it functions well -too well, in fact. Population studies carried out over the last several decades have identified a long list of human diseases that are significantly more common among individuals that carry particular HLA alleles including inflammatory, autoimmune and malignant disorders. HLAdisease association is the name of this phenomenon, and the mechanism underlying is still a subject of hot debate. Social behaviours are affected by HLA genes and preference for HLA disparate mates may provide 'good genes' for an individual's offspring. Also, certain HLA genes may be associated with shorter life and others with longer lifespan, but the effects depend both on the genetic background and on the environmental conditions. The following is a general overview of the important functional aspects of HLA in health and diseases.

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Section: Hla and Autoimmune Diseasesmentioning

confidence: 99%

Section: Hla and Autoimmune Diseasesmentioning

confidence: 99%

Clinical Role of Human Leukocyte Antigen in Health and Disease

2015

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“…Existen evidencias de la eficacia de tratamientos con ustekinumab (anticuerpo anti-IL-12p40, una de las subunidades de IL-23) y secukimumab (anticuerpo anti-IL-17) en EA, y ensayos con tofacitinib (inhibidor JAK) y fostamatinib (inhibidor TYK2) están en marcha en la actualidad. Con el objetivo de explorar nuevas terapias para pacientes con EA, especialmente para los pacientes que no responden a inhibidores de TNF-α, más estudios tienen que ser llevados a cabo 50 . Los GWAS han supuesto una herramienta vital a la hora de localizar asociaciones no-HLA en EA (Tabla 2).…”

Section: Estudios Gwasunclassified

Genética, HLA-B27 y espondilitis anquilosante: 40 años

Castro‐Santos¹,

Gutiérrez²,

Díaz‐Peña³

2014

Rev. méd. Chile

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Genetics of ankylosing spondylitis Ankylosing spondylitis (AS) is a prototypical inflammatory disease of the locomotor system affecting axial skeleton. It is part of the general group of spondyloarthopathies (SpAEpidemiología L a espondilitis anquilosante (EA) es el prototipo de las enfermedades inflamatorias del aparato locomotor que afectan al esqueleto axial y que se engloban bajo el término de espondiloartropatías (SpA). La EA es una patología de etiología desconocida cuyas principales alteraciones se producen en las zonas de inserción de ligamentos y tendones en el hueso (entesis), en la membrana sinovial y en el cartílago articular. Se considera que afecta más frecuentemente a los varones (en una relación de 3:1 respecto de las mujeres) y aparece normalmente entre los 20-30 años de vida. La prevalencia de la EA varía según zona geográfica, etnia, factores genéticos y ambientales, persistiendo aún muchos factores que se desconocen 1 . La investigación de la EA ha dado un papel fundamental al antígeno de histocompatibilidad HLA-B27, molécula capaz de acoplar un péptido en su interior que permite la posterior activación del linfocito T, y por tanto, imprescindible para el reconocimiento de lo propio y lo ajeno por parte del sistema inmune. Las diferencias en la prevalencia de HLA-B27 explican la mayor parte de la variación en la prevalencia de la EA vista en todo el mundo 2,3 . Presentar en nuestro organismo este antígeno supone una probabilidad de 1-2% de padecer EA, aunque aumenta hasta el 10-20% si, además de ser B27-positivo, existe un familiar de primer grado que ya padece la enfermedad. Lo interesante es que alrededor del 80-95% de las personas caucasoides con EA presentan positividad para HLA B27, por lo que establecer una relación entre su presencia y el desarrollo de la enfermedad ha sido el objetivo de numerosas investigaciones. En otros grupos étnicos, la relación con el HLA-B27 no es tan estrecha 1,4,5 . De este modo, sabemos que la presencia de HLA-B27 no significa que una persona padezca o vaya a padecer EA, pero en el caso de existir determinados síntomas, variaciones en parámetros bioquímicos y ciertos signos radiológicos, existiría un indicador que puede contribuir al diagnóstico definitivo, e incluso que podría ser útil en el diagnóstico diferencial de otras patologías.

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“…AS is characterized by sacroiliac joint inflammation, peripheral inflammatory arthropathy and a totally lack or low levels of rheumatoid factor (1,2). It influences EXTRA-ARTICULAR organs such as eye, skin and cardiovascular system organs less frequently.…”

mentioning

confidence: 99%

“…It influences EXTRA-ARTICULAR organs such as eye, skin and cardiovascular system organs less frequently. The prevalence of AS is about 0.1-1.4% (2). Most patients develop first symptoms in the second or third decade.…”

mentioning

confidence: 99%

Evaluation of MIF -173 G/C Polymorphism in Turkish Patients with Ankylosing Spondylitis

et al. 2016

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Background: Ankylosing spondylitis (AS) is a chronic inflammatory disease mainly affecting the spine and sacroiliac joints. Macrophage migration inhibitory (MIF) factor is a regulatory cytokine that inhibits random immune cell migration. MIF gene promoter polymorphisms play a role in the progression of several inflammatory disorders. Aims: To investigate the relationship between the MIF gene -173 G/C single-nucleotide polymorphism (SNP) and AS.

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The genetic basis of ankylosing spondylitis: new insights into disease pathogenesis

Cited by 94 publications

References 98 publications

Clinical Role of Human Leukocyte Antigen in Health and Disease

Clinical Role of Human Leukocyte Antigen in Health and Disease

Genética, HLA-B27 y espondilitis anquilosante: 40 años

Evaluation of MIF -173 G/C Polymorphism in Turkish Patients with Ankylosing Spondylitis

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