ABSTRACT
BACKGROUND AND PURPOSE: HIV-associated neurocognitive disorder still occurs despite virally suppressive combination antiretroviral therapy. In the pre-combination antiretroviral era and in patients without HIV suppression, HIV-associated neurocognitive disorder was caused by synaptodendritic injury resulting in impairment of neural networks, characterized by decreased attention, psychomotor slowing, and working memory deficits. Whether similar pathogenesis is true for HIV-associated neurocognitive disorder in the context of viral suppression is not clear. Resting-state fMRI has been shown to be efficient in detecting impaired neural networks in various neurologic illnesses. This pilot study aimed to assess resting-state functional connectivity of the brain in patients with active HIV-associated neurocognitive disorder in the context of HIV viral suppression in both blood and CSF. MATERIALS AND METHODS: Eighteen patients with active HIV-associated neurocognitive disorder (recent diagnosis with progressing symptoms) on combination antiretroviral therapy with viral suppression in both blood and CSF and 9 demographically matched control subjects underwent resting-state functional MR imaging. The connectivity in the 6 known neural networks was assessed. To localize significant ROIs within the HIV and control group, we performed a seed-based correlation for each known resting-state network. RESULTS: There were significant group differences between the control and HIV-associated neurocognitive disorder groups in the salience (0.26 versus 0.14, t = 2.6978, df = 25, P = .0123) and executive networks (0.52 versus 0.32, t = 2.2372, df = 25, P = .034). The covariate analysis with neuropsychological scores yielded statistically significant correlations in all 6 studied functional networks, with the most conspicuous correlation in salience networks. CONCLUSIONS: Active HIV-associated neurocognitive disorder in virally suppressed patients is associated with significantly decreased connectivity in the salience and executive networks, thereby making it potentially useful as a biomarker.
Subject(s)
AIDS Dementia Complex/diagnostic imaging , HIV Infections/diagnostic imaging , Nerve Net/diagnostic imaging , AIDS Dementia Complex/pathology , AIDS Dementia Complex/psychology , Antiretroviral Therapy, Highly Active , Brain/diagnostic imaging , Executive Function , HIV Infections/pathology , HIV Infections/virology , Humans , Image Processing, Computer-Assisted , Magnetic Resonance Imaging , Male , Middle Aged , Nerve Net/pathology , Neurocognitive Disorders/diagnostic imaging , Neurocognitive Disorders/pathology , Neurocognitive Disorders/psychology , Neuropsychological Tests , Pilot Projects , RestABSTRACT
Polysplenia, as part of the heterotaxy syndrome, is a rare embryological disorder which results from failure of development of the usual left-right asymmetry of organs. It is often associated with cardiac and biliary abnormalities, which are the usual causes of death in early neonatal life. A congenitally short pancreas and abnormalities with portal vein formation, gut malrotations and inferior vena cava anomalies are known to be associated with this rare syndrome. We report a case of polysplenia in an adult female presenting with obstructive jaundice owing to choledocholithiasis, possibly formed by biliary stasis as a result of compression of the common bile duct by the preduodenal portal vein, and review the literature. The patient was also found to have complete agenesis of the dorsal pancreas on CT and endoscopic retrograde cholangiopancreatography.
Subject(s)
Heterotaxy Syndrome/diagnostic imaging , Jaundice, Obstructive/diagnostic imaging , Pancreas/diagnostic imaging , Portal Vein/diagnostic imaging , Spleen/diagnostic imaging , Tomography, X-Ray Computed , Choledocholithiasis/complications , Female , Heterotaxy Syndrome/surgery , Humans , Jaundice, Obstructive/etiology , Middle Aged , Pancreas/abnormalities , Portal Vein/abnormalities , Spleen/abnormalitiesSubject(s)
Abscess/diagnosis , Diffusion Magnetic Resonance Imaging , Mucormycosis/diagnosis , Sinusitis/diagnosis , Trigeminal Nerve Diseases/diagnosis , Abscess/microbiology , Craniotomy , Diagnosis, Differential , Humans , Male , Middle Aged , Mucormycosis/microbiology , Mucormycosis/physiopathology , Sinusitis/microbiology , Sinusitis/physiopathology , Trigeminal Nerve Diseases/microbiology , Trigeminal Nerve Diseases/physiopathologyABSTRACT
BACKGROUND: Pathophysiological basis of Magnetisation Transfer Ratio (MTR) reduction in multiple sclerosis still remains a matter of controversy. Optic nerve represents an ideal model to study the consequences of axonal loss and demyelination on MTR since effects of disease on the optic nerve are clinically apparent and potentially quantifiable by objective means. By measuring the latency of multifocal visual evoked potentials (mfVEP) (measure of optic nerve conduction) and Retinal Nerve Fiber Layer (RNFL) thickness (measure of axonal damage) we investigated the effect of neurodegeneration and demyelination on MTR after an episode of optic neuritis (ON). METHODS: 23 patients with a single unilateral episode of ON and 10 healthy volunteers were enrolled. Orbital MRI including MTR protocol, Optical Coherence Tomography and Multifocal VEP were performed at post-acute stage of ON. RESULTS: Average MTR of affected eye was significantly reduced as compared to the fellow eye and normal controls. There was a highly significant correlation between MTR and measures of axonal loss (RNFL thickness and mfVEP amplitude), which was independent on the level of demyelination. While latency delay also correlated significantly with MTR, correlation became non-significant when adjusted for the degree of axonal loss. There was a significant reduction of MTR in a group of patients with extensive axonal damage, while MTR remained normal in a group of patients with extensive demyelination, but little or no axonal loss. CONCLUSION: Results of this study indicate that reduction of optic nerve MTR after an episode of ON has a strong association with the degree of axonal damage, but not with demyelination.
