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Detection of clinically relevant molecular alterations in Chronic Lymphocytic Leukaemia by Nanopore sequencing


Chronic lymphocytic leukaemia (CLL) is the most prevalent form of leukaemia in the Western world, and displays considerable biological and clinical heterogeneity. CLL can progress into either an aggressive, chemo-resistant form with poor prognosis, or an indolent form with a similar life-expectancy to that of the general population. A number of prognostic markers, in particular IgHV mutation status, mutations in the TP53 gene and deletions of the p-arm of chromosome 17, can be used to predict a patient’s response to individual chemo-therapeutics and give an indication as to their long-term prognosis. Clinical guidelines recommend screening patients prior to the initial, and any subsequent, rounds of treatment. Current screening methods involve three separate assays, each of which is time-consuming and requires significant investment in equipment. Nanopore sequencing offers a rapid, low-cost alternative, with the potential to generate a full prognostic dataset in a single assay.

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