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Review
. 2019 Nov;104(11):2135-2143.
doi: 10.3324/haematol.2018.207506. Epub 2019 Oct 3.

How I diagnose and manage Philadelphia chromosome-like acute lymphoblastic leukemia

Avraham Frisch  1 Yishai Ofran  2   3
Affiliations
Review

How I diagnose and manage Philadelphia chromosome-like acute lymphoblastic leukemia

Avraham Frisch et al. Haematologica. 2019 Nov.

Abstract

Advances in our understanding of mechanisms of leukemogenesis and driver mutations in acute lymphoblastic leukemia (ALL) lead to a more precise and informative sub-classification, mainly of B-cell ALL. In parallel, in recent years, novel agents have been approved for the therapy of B-cell ALL, and many others are in active clinical research. Among the newly recognized disease subtypes, Philadelphia-chromosome-like ALL is the most heterogeneous and thus, diagnostically challenging. Given that this subtype of B-cell ALL is associated with a poorer prognosis, improvement of available therapeutic approaches and protocols is a burning issue. Herein, we summarize, in a clinically relevant manner, up-to-date information regarding diagnostic strategies developed for the identification of patients with Philadelphia-chromosome-like ALL. Common therapeutic dilemmas, presented as several case scenarios, are also discussed. It is currently acceptable that patients with B-cell ALL, treated with an aim of cure, irrespective of their age, be evaluated for a Philadelphia-chromosome-like signature as early as possible. Following Philadelphia-chromosome-like recognition, a higher risk of resistance or relapse must be realized and treatment should be modified based on the patient's specific genetic driver and clinical features. However, while active targeted therapeutic options are limited, there is much more to do than just prescribe a matched inhibitor to the identified mutated driver genes. In this review, we present a comprehensive evidence-based approach to the diagnosis and management of Philadelphia-chromosome-like ALL at different time-points during the disease course.

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Figures

Figure 1.
Figure 1.
Screening of newly diagnosed cases of B-cell other acute lymphoblastic leukemia. *FISH-break-apart. **Targeted sequencing for mutations in JAK, IL7R, FLT3, SH2B3, RAS and PTPN11. ALL: acute lymphoblastic leukemia; LDA: low density microarray; FISH: fluorescence in situ hybridization; Ph-like: Philadelphia chromosome like.
See this image and copyright information in PMC

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