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Discovery and Elucidation of the mechanisms of Action of Tumour Selective Compunds – Sonia Lain Group

Discovery and elucidation of the mechanisms of action of tumour selective compunds.

An illustration from Sonia Lain Group
An illustration from Sonia Lain Group

Our research

Aside from blood cancer cells, several cell lines from solid cancers respond to DHODH inhibitors in culture. However, the results in vivo are less impressive. One possible reason for this is that the levels of uridine in plasma can supplement UMP production and therefore rescue cells from DHODH inhibition.

After identifying a number of potent and specific inhibitors of DHODH, our current research is devoted to finding strategies to improve their therapeutic index for cancer treatment. This is performed by identifying agents that rescue normal cells from DHODH blockage (including T cells and their antitumour function), determining which tumor types are hypersensitive to inhibition of this key enzyme and by elucidating the reasons for this hypersensitivity at the molecular level.

Discovery and elucidation of the mechanisms of action of tumour selective compounds

Activating p53 has long been considered as an attractive strategy to treat cancer. Since 2004, the most specific approach to activate wildtype p53 without damaging DNA is to use inhibitors of mdm2 with peptides or small molecules such as nutlin3 (Vassilev et al., Science, 2004).  However, and in spite of the enormous efforts of academia and industry, mdm2 inhibitors have yet to deliver in the clinic. This slow progress may be due to lack of selectivity for cancer cells or because many cancer cell types tend to undergo a reversible cell cycle arrest. An additional concern is that mdm2 inhibitors such as nutlin3 can lead a significant proportion of cells to accumulate in G2. This effect, which also occurs in cultures of normal cells such as primary fibroblasts could have undesired  consequences. Indeed, as demonstrated by others and confirmed by us, when the mdm2 inhibitor is removed G2 cells can enter S phase leading to the appearance of 8N cells and increasing the risk of genome instability.

Although less selective for the p53 pathway than mdm2 inhibitors, numerous other small molecules activating wild type p53 have been described in our lab. Of these, a large number happen to be inhibitors of the enzyme dihydroorotate dehydrogenase DHODH, a mitochondrial enzyme coupled to the electron transport chain that is involved in the de novo synthesis of uridine 5’-monophosphate (UMP) and therefore, of all pyrimidine ribonucleotides. As such, DHODH inhibitors target highly proliferating cells (including activated T cells) and are therefore used in the clinic for the control of autoimmune diseases and are in clinical trial as antivirals. With regards to cancer, it is well established that inhibition of UMP synthesis can lead to the accumulation of cancer cells in S phase, a very vulnerable stage of the cell cycle and where p53 activation may cause cell death more easily. In addition, DHODH inhibitors can promote differentiation of leukemic cells, which is why several DHODH inhibitors have entered clinical trials for acute myeloid leukemia.

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Publications

Selected publications

  • Article: ISCIENCE. 2021;24(5):102494
    Zhang J; Teran G; Popa M; Madapura H; Ladds MJGW; Lianoudaki D; Grunler J; Arsenian-Henriksson M; McCormack E; Rottenberg ME; Catrina S-B; Lain S; Darekar S
  • Article: JOURNAL OF MEDICINAL CHEMISTRY. 2020;63(8):3915-3934
    Popova G; Ladds MJGW; Johansson L; Saleh A; Larsson J; Sandberg L; Sahlberg SH; Qian W; Gullberg H; Garg N; Gustavsson A-L; Haraldsson M; Lane D; Yngve U; Lain S
  • Review: CANCER & METABOLISM. 2020;8(1):12
    Mollick T; Lain S
  • Article: CLINICAL GENETICS. 2019;96(3):216-225
    Kharaziha P; Ceder S; Axell O; Krall M; Fotouhi O; Bohm S; Lain S; Borg A; Larsson C; Wiman KG; Tham E; Bajalica-Lagercrantz S
  • Review: JOURNAL OF MOLECULAR CELL BIOLOGY. 2019;11(3):245-254
    Ladds MJGW; Lain S
  • Article: JOURNAL OF PHYSICAL CHEMISTRY LETTERS. 2018;9(14):4082-4086
    Gault J; Lianoudaki D; Kaldmae M; Kronqvist N; Rising A; Johansson J; Lohkamp B; Lain S; Allison TM; Lane DP; Marklund EG; Landreh M
  • Article: NATURE COMMUNICATIONS. 2018;9(1):1107
    Ladds MJGW; van Leeuwen IMM; Drummond CJ; Chu S; Healy AR; Popova G; Fernandez AP; Mollick T; Darekar S; Sedimbi SK; Nekulova M; Sachweh MCC; Campbell J; Higgins M; Tuck C; Popa M; Safont MM; Gelebart P; Fandalyuk Z; Thompson AM; Svensson R; Gustavsson A-L; Johansson L; Farnegardh K; Yngve U; Saleh A; Haraldsson M; D'Hollander ACA; Franco M; Zhao Y; Hakansson M; Walse B; Larsson K; Peat EM; Pelechano V; Lunec J; Vojtesek B; Carmena M; Earnshaw WC; McCarthy AR; Westwood NJ; Arsenian-Henriksson M; Lane DP; Bhatia R; McCormack E; Lain S
  • Article: CELL CHEMICAL BIOLOGY. 2018;25(3):309-317.e4
    Costeira-Paulo J; Gault J; Popova G; Ladds MJGW; van Leeuwen IMM; Sarr M; Olsson A; Lane DP; Lain S; Marklund EG; Landreh M
  • Article: PLOS ONE. 2018;13(4):e0195956
    Ladds MJGW; Pastor-Fernandez A; Popova G; van Leeuwen IMM; Eng KE; Drummond CJ; Johansson L; Svensson R; Westwood NJ; McCarthy AR; Tholander F; Popa M; Lane DP; McCormack E; McInerney GM; Bhatia R; Lain S
  • Article: CELL CYCLE. 2016;15(9):1267-1275
    Madapura HS; Salamon D; Wiman KG; Lain S; Klein E; Nagy N
  • Article: ONCOTARGET. 2015;6(18):16488-16506
    Sachweh MCC; Stafford WC; Drummond CJ; McCarthy AR; Higgins M; Campbell J; Brodin B; Arner ESJ; Lain S
  • Article: NATURE BIOTECHNOLOGY. 2015;33(4):415-423
    Scholz C; Weinert BT; Wagner SA; Beli P; Miyake Y; Qi J; Jensen LJ; Streicher W; McCarthy AR; Westwood NJ; Lain S; Cox J; Matthias P; Mann M; Bradner JE; Choudhary C
  • Article: CELL DEATH AND DISEASE. 2014;5(10):e1483
    Ma L; Maruwge W; Strambi A; D'Arcy P; Pellegrini P; Kis L; de Milito A; Lain S; Brodin B
  • Article: CELL STEM CELL. 2014;15(4):431-446
    Li L; Osdal T; Ho Y; Chun S; McDonald T; Agarwal P; Lin A; Chu S; Qi J; Li L; Hsieh Y-T; Dos Santos C; Yuan H; Ha T-Q; Popa M; Hovland R; Bruserud O; Gjertsen BT; Kuo Y-H; Chen W; Lain S; McCormack E; Bhatia R
  • Article: MOLECULAR CANCER THERAPEUTICS. 2013;12(4):471-480
    van Leeuwen IMM; Higgins M; Campbell J; McCarthy AR; Sachweh MCC; Navarro AM; Lain S
  • Article: MOLECULAR CANCER THERAPEUTICS. 2013;12(4):352-360
    McCarthy AR; Sachweh MCC; Higgins M; Campbell J; Drummond CJ; van Leeuwen IMM; Pirrie L; Ladds MJGW; Westwood NJ; Lain S
  • Article: CELL DEATH AND DISEASE. 2013;4(3):e533
    Sachweh MCC; Drummond CJ; Higgins M; Campbell J; Lain S
  • Article: SCIENTIFIC REPORTS. 2013;3:1275
    MacCallum SF; Groves MJ; James J; Murray K; Appleyard V; Prescott AR; Drbal AA; Nicolaou A; Cunningham J; Haydock S; Ganley IG; Westwood NJ; Coates PJ; Lain S; Tauro S
  • Article: CELL CYCLE. 2012;11(24):4563-4569
    Madapura HS; Salamon D; Wiman KG; Lain S; Klein G; Klein E; Nagy N
  • Article: CELL CYCLE. 2012;11(9):1851-1861
    van Leeuwen IMM; Rao B; Sachweh MCC; Lain S
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