Diagnosis and Management of Posterior Cortical Atrophy

Author:

Yong Keir X. X.ORCID,Graff-Radford Jonathan,Ahmed Samrah,Chapleau Marianne,Ossenkoppele Rik,Putcha Deepti,Rabinovici Gil D.,Suarez-Gonzalez Aida,Schott Jonathan M.,Crutch Sebastian,Harding Emma

Abstract

Abstract Purpose of review The study aims to provide a summary of recent developments for diagnosing and managing posterior cortical atrophy (PCA). We present current efforts to improve PCA characterisation and recommendations regarding use of clinical, neuropsychological and biomarker methods in PCA diagnosis and management and highlight current knowledge gaps. Recent findings Recent multi-centre consensus recommendations provide PCA criteria with implications for different management strategies (e.g. targeting clinical features and/or disease). Studies emphasise the preponderance of primary or co-existing Alzheimer’s disease (AD) pathology underpinning PCA. Evidence of approaches to manage PCA symptoms is largely derived from small studies. Summary PCA diagnosis is frequently delayed, and people are likely to receive misdiagnoses of ocular or psychological conditions. Current treatment of PCA is symptomatic — pharmacological and non-pharmacological — and the use of most treatment options is based on small studies or expert opinion. Recommendations for non-pharmacological approaches include interdisciplinary management tailored to the PCA clinical profile — visual-spatial — rather than memory-led, predominantly young onset — and psychosocial implications. Whilst emerging disease-modifying treatments have not been tested in PCA, an accurate and timely diagnosis of PCA and determining underlying pathology is of increasing importance in the advent of disease-modifying therapies for AD and other albeit rare causes of PCA.

Funder

Alzheimer's Society

NIH Clinical Center

Wellcome Trust

Alzheimer's Association

ESRC-NIHR

NIHR

Economic and Social Research Council

Alzheimer Society

Publisher

Springer Science and Business Media LLC

Subject

Neurology (clinical)

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