The PIP4K2 inhibitor THZ-P1-2 exhibits antileukemia activity by disruption of mitochondrial homeostasis and autophagy

Abstract: Treatment of acute leukemia is challenging due to genetic heterogeneity between and even within patients. Leukemic stem cells (LSCs) are relatively drug-resistant and frequently lead to relapse. Their plasticity and capacity to adapt to extracellular stress, in which mitochondrial metabolism and autophagy play important roles, further complicates treatment. Genetic models of phosphatidylinositol-5-phosphate 4-kinase type 2 proteins (PIP4K2s) inhibition demonstrated the relevance of these enzymes in mitochondri… Show more

“…17 Various PI5P4K inhibitors have been reported to have a therapeutic effect in oncology settings. 18,19 Covalent pan-PI5P4K inhibitor THZ-P1-2 (1) was shown to have antiproliferative activity in acute myeloid and lymphoblastic leukaemias (AML/ALL) [19][20][21][22] and the small molecule A131 (2), which was shown to target mitotic pathways and PI5P4Ks, was effective in cancer cell-specific lethality 18 (Fig. 1).…”

Identification of ARUK2002821 as an isoform-selective PI5P4Kα inhibitor

“…17 Various PI5P4K inhibitors have been reported to have a therapeutic effect in oncology settings. 18,19 Covalent pan-PI5P4K inhibitor THZ-P1-2 (1) was shown to have antiproliferative activity in acute myeloid and lymphoblastic leukaemias (AML/ALL) [19][20][21][22] and the small molecule A131 (2), which was shown to target mitotic pathways and PI5P4Ks, was effective in cancer cell-specific lethality 18 (Fig. 1).…”

Identification of ARUK2002821 as an isoform-selective PI5P4Kα inhibitor

“…Both PI5P4Kα and PI5P4Kβ are involved in p53-deficient breast cancer and soft tissue sarcomas 22,23 and high expression of both PI5P4Kα and PI5P4Kγ associate with unfavourable clinical outcome in AML. 24 Several recent reports detail inhibitors for PI5P4Ks, not only pan-specific [25][26][27][28][29] but also isoform specific. [30][31][32][33][34] Emerging tools are also being developed for dual-specific inhibitors for PI5P4Kα and PI5P4Kβ 22,35 and methods have also been reported for removing protein completely in cells using PROTAC systems, such as JWZ-1-80 for PI5P4Kγ, 36 which will be useful to interrogate non-catalytic roles.…”

The rational design of ARUK2007145, a dual inhibitor of the α and γ isoforms of the lipid kinase phosphatidylinositol 5-phosphate 4-kinase (PI5P4K)