2008
DOI: 10.1016/j.nbd.2008.01.012
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Immune transcriptome alterations in the temporal cortex of subjects with autism

Abstract: Autism is a severe disorder that involves both genetic and environmental factors. Expression profiling of the superior temporal gyrus of six autistic subjects and matched controls revealed increased transcript levels of many immune system related genes. We also noticed changes in transcripts related to cell communication, differentiation, cell cycle regulation and chaperone systems. Critical expression changes were confirmed by qPCR (BCL6, CHI3L1, CYR61, IFI16, IFITM3, MAP2K3, PTDSR, RFX4, SPP1, RELN, NOTCH2,… Show more

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Cited by 355 publications
(306 citation statements)
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“…54,55 These proinflammatory effects of PKCb sharply contrast with the decrease in PRKCB1 gene expression reported here, because the very same neocortical brain samples employed in this study display enhanced oxidative stress (L Palmieri, AM Persico et al, submitted) and increased immune gene expression. 56 The latter results are in agreement with previous studies demonstrating enhanced oxidative stress in autism 57 and an ongoing immune reaction in a set of postmortem brain tissue samples of autistic patients largely non-overlapping with ours, and in the CSF of autistic children collected in vivo. 58 …”
Section: Discussionsupporting
confidence: 93%
“…54,55 These proinflammatory effects of PKCb sharply contrast with the decrease in PRKCB1 gene expression reported here, because the very same neocortical brain samples employed in this study display enhanced oxidative stress (L Palmieri, AM Persico et al, submitted) and increased immune gene expression. 56 The latter results are in agreement with previous studies demonstrating enhanced oxidative stress in autism 57 and an ongoing immune reaction in a set of postmortem brain tissue samples of autistic patients largely non-overlapping with ours, and in the CSF of autistic children collected in vivo. 58 …”
Section: Discussionsupporting
confidence: 93%
“…According to post-mortem and in vivo studies, an ongoing immune response could provide such a contribution by raising intracellular Ca 2 þ levels through cytokines, such as tumor necrosis factor-a and receptors, like CD38. 28,47,48 Indeed, the existence of an immune dysreactivity is also supported by the association between macrocephaly and macrosomy in autism with a history of immune/ allergic disorders, either in the patient or in his/her first-degree relatives. 9 Immune mechanisms may also mediate the vulnerability to autism conferred by recently described 16p11.2 microdeletions.…”
Section: à1688mentioning
confidence: 96%
“…The same, or slightly larger paired patient-control samples, have been the object of recent reports. [26][27][28] Brain tissue processing Fresh frozen brain tissue samples dissected from the superior temporal gyrus (BA 41/42 or 22) of patients and controls were obtained through the Autism Tissue Program from the NICHD Brain and Tissue Bank and the Harvard Brain Tissue Resource Center. Cortical gray matter (100-200 mg) was suspended in a buffer containing 250 mM sucrose and 10 mM TRIS, pH 7.4 and homogenated using a Teflon glass potter.…”
Section: Patient Brain Tissue Informationmentioning
confidence: 99%
“…In between these extremes, ASD for most cases fully qualifies for the definition of a Bcomplex^disorder, whereby a host of rare and common genetic variants, often but not necessarily in conjunction with epigenetic factors [63], yield the neurodevelopmental abnormalities summarized above, resulting in autistic behaviors. Finally, neuroinflammation is also a frequent finding in postmortem brains of autistic individuals [64,65]. It may represent a nonspecific consequence of insufficient neurite pruning and abnormal wiring of neural networks, resulting in elevated oxidative stress (possibly a common feature shared by several neurodevelopmental disorders) [66], but it could also stem from a broader immune dysfunction which, together with gastrointestinal disturbances and recurrent infections, collectively qualifies ASD as a systemic disorder [67][68][69][70][71].…”
Section: Autism Spectrum Disorder: Clinical Traits Neuropsychologicamentioning
confidence: 99%