Detail
Article
Online article
FT
Medvik - BMC
  • Something wrong with this record ?

BH3 Mimetics in Hematologic Malignancies

P. Klener, D. Sovilj, N. Renesova, L. Andera

. 2021 ; 22 (18) : . [pub] 20210921

Language English Country Switzerland

Document type Journal Article, Review

Persistent link   https://www.medvik.cz/link/bmc22003694

Grant support
AZV NU21-03-00386 Agentura Pro Zdravotnický Výzkum České Republiky
GACR17-14007S and GACR19-08772S Grantová Agentura České Republiky
Center of Excellence UNCE/MED/016 Univerzita Karlova v Praze
PROGRES Q26/LF1 and PROGRES Q28/LF1 Ministerstvo Školství, Mládeže a Tělovýchovy

Hematologic malignancies (HM) comprise diverse cancers of lymphoid and myeloid origin, including lymphomas (approx. 40%), chronic lymphocytic leukemia (CLL, approx. 15%), multiple myeloma (MM, approx. 15%), acute myeloid leukemia (AML, approx. 10%), and many other diseases. Despite considerable improvement in treatment options and survival parameters in the new millennium, many patients with HM still develop chemotherapy‑refractory diseases and require re-treatment. Because frontline therapies for the majority of HM (except for CLL) are still largely based on classical cytostatics, the relapses are often associated with defects in DNA damage response (DDR) pathways and anti-apoptotic blocks exemplified, respectively, by mutations or deletion of the TP53 tumor suppressor, and overexpression of anti-apoptotic proteins of the B-cell lymphoma 2 (BCL2) family. BCL2 homology 3 (BH3) mimetics represent a novel class of pro-apoptotic anti-cancer agents with a unique mode of action-direct targeting of mitochondria independently of TP53 gene aberrations. Consequently, BH3 mimetics can effectively eliminate even non-dividing malignant cells with adverse molecular cytogenetic alterations. Venetoclax, the nanomolar inhibitor of BCL2 anti-apoptotic protein has been approved for the therapy of CLL and AML. Numerous venetoclax-based combinatorial treatment regimens, next-generation BCL2 inhibitors, and myeloid cell leukemia 1 (MCL1) protein inhibitors, which are another class of BH3 mimetics with promising preclinical results, are currently being tested in several clinical trials in patients with diverse HM. These pivotal trials will soon answer critical questions and concerns about these innovative agents regarding not only their anti-tumor efficacy but also potential side effects, recommended dosages, and the optimal length of therapy as well as identification of reliable biomarkers of sensitivity or resistance. Effective harnessing of the full therapeutic potential of BH3 mimetics is a critical mission as it may directly translate into better management of the aggressive forms of HM and could lead to significantly improved survival parameters and quality of life in patients with urgent medical needs.

References provided by Crossref.org

000      
00000naa a2200000 a 4500
001      
bmc22003694
003      
CZ-PrNML
005      
20220127145956.0
007      
ta
008      
220113s2021 sz f 000 0|eng||
009      
AR
024    7_
$a 10.3390/ijms221810157 $2 doi
035    __
$a (PubMed)34576319
040    __
$a ABA008 $b cze $d ABA008 $e AACR2
041    0_
$a eng
044    __
$a sz
100    1_
$a Klener, Pavel $u First Department of Internal Medicine‑Hematology, General University Hospital in Prague, 121 08 Prague, Czech Republic $u First Faculty of Medicine, Institute of Pathological Physiology, Charles University, 121 08 Prague, Czech Republic
245    10
$a BH3 Mimetics in Hematologic Malignancies / $c P. Klener, D. Sovilj, N. Renesova, L. Andera
520    9_
$a Hematologic malignancies (HM) comprise diverse cancers of lymphoid and myeloid origin, including lymphomas (approx. 40%), chronic lymphocytic leukemia (CLL, approx. 15%), multiple myeloma (MM, approx. 15%), acute myeloid leukemia (AML, approx. 10%), and many other diseases. Despite considerable improvement in treatment options and survival parameters in the new millennium, many patients with HM still develop chemotherapy‑refractory diseases and require re-treatment. Because frontline therapies for the majority of HM (except for CLL) are still largely based on classical cytostatics, the relapses are often associated with defects in DNA damage response (DDR) pathways and anti-apoptotic blocks exemplified, respectively, by mutations or deletion of the TP53 tumor suppressor, and overexpression of anti-apoptotic proteins of the B-cell lymphoma 2 (BCL2) family. BCL2 homology 3 (BH3) mimetics represent a novel class of pro-apoptotic anti-cancer agents with a unique mode of action-direct targeting of mitochondria independently of TP53 gene aberrations. Consequently, BH3 mimetics can effectively eliminate even non-dividing malignant cells with adverse molecular cytogenetic alterations. Venetoclax, the nanomolar inhibitor of BCL2 anti-apoptotic protein has been approved for the therapy of CLL and AML. Numerous venetoclax-based combinatorial treatment regimens, next-generation BCL2 inhibitors, and myeloid cell leukemia 1 (MCL1) protein inhibitors, which are another class of BH3 mimetics with promising preclinical results, are currently being tested in several clinical trials in patients with diverse HM. These pivotal trials will soon answer critical questions and concerns about these innovative agents regarding not only their anti-tumor efficacy but also potential side effects, recommended dosages, and the optimal length of therapy as well as identification of reliable biomarkers of sensitivity or resistance. Effective harnessing of the full therapeutic potential of BH3 mimetics is a critical mission as it may directly translate into better management of the aggressive forms of HM and could lead to significantly improved survival parameters and quality of life in patients with urgent medical needs.
650    _2
$a zvířata $7 D000818
650    _2
$a apoptóza $x fyziologie $7 D017209
650    _2
$a biologické markery $x metabolismus $7 D015415
650    _2
$a bicyklické sloučeniny heterocyklické $x terapeutické užití $7 D019086
650    _2
$a poškození DNA $x účinky léků $x genetika $7 D004249
650    _2
$a hematologické nádory $x farmakoterapie $x metabolismus $7 D019337
650    _2
$a lidé $7 D006801
650    _2
$a sulfonamidy $x terapeutické užití $7 D013449
650    _2
$a nádorový supresorový protein p53 $x metabolismus $7 D016159
655    _2
$a časopisecké články $7 D016428
655    _2
$a přehledy $7 D016454
700    1_
$a Sovilj, Dana $u Institute of Biotechnology CAS/BIOCEV, 252 50 Vestec, Czech Republic
700    1_
$a Renesova, Nicol $u First Faculty of Medicine, Institute of Pathological Physiology, Charles University, 121 08 Prague, Czech Republic
700    1_
$a Andera, Ladislav $u Institute of Biotechnology CAS/BIOCEV, 252 50 Vestec, Czech Republic $u Institute of Molecular Genetics CAS, 142 20 Prague, Czech Republic
773    0_
$w MED00176142 $t International journal of molecular sciences $x 1422-0067 $g Roč. 22, č. 18 (2021)
856    41
$u https://pubmed.ncbi.nlm.nih.gov/34576319 $y Pubmed
910    __
$a ABA008 $b sig $c sign $y p $z 0
990    __
$a 20220113 $b ABA008
991    __
$a 20220127145952 $b ABA008
999    __
$a ok $b bmc $g 1751217 $s 1154843
BAS    __
$a 3
BAS    __
$a PreBMC
BMC    __
$a 2021 $b 22 $c 18 $e 20210921 $i 1422-0067 $m International journal of molecular sciences $n Int J Mol Sci $x MED00176142
GRA    __
$a AZV NU21-03-00386 $p Agentura Pro Zdravotnický Výzkum České Republiky
GRA    __
$a GACR17-14007S and GACR19-08772S $p Grantová Agentura České Republiky
GRA    __
$a Center of Excellence UNCE/MED/016 $p Univerzita Karlova v Praze
GRA    __
$a PROGRES Q26/LF1 and PROGRES Q28/LF1 $p Ministerstvo Školství, Mládeže a Tělovýchovy
LZP    __
$a Pubmed-20220113

Find record

Citation metrics

Archiving options