von Hippel-Lindau (VHL)

The von Hippel-Lindau (VHL) protein functions as a tumor suppressor and substrate recognition subunit of the Cullin2-RING E3 ligase complex (CRL2^VHL), mediating oxygen-sensing by targeting hypoxia-inducible factor alpha (HIF-α) for ubiquitination and proteasomal degradation^[1]^[2]. Loss or mutation of VHL disrupts HIF-α regulation, resulting in differential activation of HIF isoforms, where HIF-1α can suppress and HIF-2α can promote tumorigenesis^[3]^[4]^[5]. Mechanistically, VHL-mediated ubiquitination specifically regulates HIF-2α-driven transcriptional programs that control cell proliferation, angiogenesis, and erythropoiesis, as demonstrated in VHL-R200W polycythemia models and renal cell carcinoma (RCC) studies^[6]^[7]^[8]. Compared with related isoforms, HIF-2α exhibits tissue-specific oncogenic activity, particularly in proximal tubular epithelial cells, whereas HIF-1α exhibits tumor-suppressive effects^[4]^[9]^[10]. Experimental models, including zebrafish and conditional mouse knockouts, recapitulate VHL loss phenotypes such as hemangioblastomas, impaired visual function, and splenic erythropoiesis, facilitating pharmacological intervention studies^[11]^[12]^[13]. VHL-targeted small molecules, such as VH298 and belzutifan, stabilize VHL protein or inhibit HIF-2α activity, thereby modulating downstream hypoxia responses and providing a framework for therapeutic strategies in VHL-associated RCC and other neoplasms^[1]^[14]^[15]. Overall, precise regulation of VHL and HIF isoforms underpins disease pathogenesis, isoform-specific biology, and translational applications in inhibitor or agonist development^[2]^[4]^[9].

References:

[1]. Rabezanahary H, et al. Live virus neutralizing antibodies against pre and post Omicron strains in food and retail workers in Québec, Canada. Heliyon. 2024 May 21;10(10):e31026. [Content Brief]

[2]. Takamori H, et al. Development of drugs targeting hypoxia-inducible factor against tumor cells with VHL mutation: Story of 127 years. Cancer Sci. 2023 Apr;114(4):1208-1217. [Content Brief]

[3]. Schödel J, et al. Hypoxia, Hypoxia-inducible Transcription Factors, and Renal Cancer. Eur Urol. 2016 Apr;69(4):646-657. [Content Brief]

[4]. Lima JDCC, et al. HIFα isoform specific activities drive cell-type specificity of VHL-associated oncogenesis. Nat Commun. 2025 Oct 16;16(1):9185. [Content Brief]

[5]. Mazumder S, et al. Downstream Targets of VHL/HIF-α Signaling in Renal Clear Cell Carcinoma Progression: Mechanisms and Therapeutic Relevance. Cancers (Basel). 2023 Feb 19;15(4):1316. [Content Brief]

[6]. Hickey MM, et al. von Hippel-Lindau mutation in mice recapitulates Chuvash polycythemia via hypoxia-inducible factor-2alpha signaling and splenic erythropoiesis. J Clin Invest. 2007 Dec;117(12):3879-89. [Content Brief]

[7]. Ding Z, et al. Genetic and pharmacological strategies to refunctionalize the von Hippel Lindau R167Q mutant protein. Cancer Res. 2014 Jun 1;74(11):3127-36. [Content Brief]

[8]. Cautain B, et al. Identification of the Lipodepsipeptide MDN-0066, a Novel Inhibitor of VHL/HIF Pathway Produced by a New Pseudomonas Species. PLoS One. 2015 May 27;10(5):e0125221. [Content Brief]

[9]. Lee SJ, et al. Von Hippel-Lindau tumor suppressor gene loss in renal cell carcinoma promotes oncogenic epidermal growth factor receptor signaling via Akt-1 and MEK-1. Eur Urol. 2008 Oct;54(4):845-53. [Content Brief]

[10]. Hermans A, et al. A 3D-Printed and Freely Available Device to Measure the Zebrafish Optokinetic Response Before and After Injury. Zebrafish. 2024 Apr;21(2):144-148. [Content Brief]

[11]. Abimbola A, et al. Role of Targeted Therapy in the Management of von Hippel-Lindau Disease-Associated Renal Cell Carcinoma: A Single-Proportion Meta-Analysis. Cureus. 2025 Nov 23;17(11):e97606. [Content Brief]

[12]. Kaelin WG Jr. Von Hippel-Lindau disease: insights into oxygen sensing, et al. Von Hippel-Lindau disease: insights into oxygen sensing, protein degradation, and cancer. J Clin Invest. 2022 Sep 15;132(18):e162480. [Content Brief]

[13]. Soares P, et al. Group-Based Optimization of Potent and Cell-Active Inhibitors of the von Hippel-Lindau (VHL) E3 Ubiquitin Ligase: Structure-Activity Relationships Leading to the Chemical Probe (2S,4R)-1-((S)-2-(1-Cyanocyclopropanecarboxamido)-3,3-dimethylbutanoyl)-4-hydroxy-N-(4-(4-methylthiazol-5-yl)benzyl)pyrrolidine-2-carboxamide (VH298). J Med Chem. 2018 Jan 25;61(2):599-618. [Content Brief]

[14]. Steenhard BM, et al. Deletion of von Hippel-Lindau in glomerular podocytes results in glomerular basement membrane thickening, ectopic subepithelial deposition of collagen {alpha}1{alpha}2{alpha}1(IV), expression of neuroglobin, and proteinuria. Am J Pathol. 2010 Jul;177(1):84-96. [Content Brief]

von Hippel-Lindau (VHL) Control (1)

von Hippel-Lindau (VHL) Verwandte Produkte (79):

By Type:	Pan (2) Selective (55)

Art. -Nr.	Produktname	CAS. Nr.	Reinheit	Chemische Struktur

HY-W584528

VH032 analogue-2	1448189-66-9
VH032 analogue-2 is a VH032 (HY-120217) analog that acts as a ligand for VHL, recruiting von Hippel-Lindau (VHL) protein. VH032 analogue-2 will remove the protective group under acidic conditions, and can be directly used for the synthesis of PROTAC molecules. VH032 analogue-2 is a key intermediate for the synthesis of PROTACs based on VHL ligands.

HY-W584534

VH032-CH2-Boc	2827750-24-1
VH032-CH2-Boc is a Boc-modified VH032 (HY-120217) that serves as a ligand for VHL and recruits von Hippel-Lindau (VHL) proteins. VH032-CH2-Boc will remove the protecting group under acidic conditions and be directly used in PROTAC molecule synthesis. VH032-CH2-Boc is a key intermediate in the synthesis of PROTAC based on VHL ligand.

HY-112078A

(S,R,S,R)-AHPC-Me	2055344-67-5
(S,R,S,R)-AHPC-Me serves as a VHL ligand that facilitates the recruitment of the VHL protein.

HY-168699

E3 ligase Ligand 45
E3 ligase Ligand 45 is an E3 ligase ligand that can be used to synthesize the PROTAC degrader Setidegrasib (HY-148273) for Ras.

HY-W584527

VH032 analogue-1	2111829-84-4
VH032 analogue-1 is a VH032 (HY-120217) analog that acts as a ligand for VHL, recruiting von Hippel-Lindau (VHL) protein. VH032 analogue-1 will remove the protective group under acidic conditions and be directly used for PROTAC molecular synthesis. VH032 analogue-1 is a key intermediate in the synthesis of PROTACs based on VHL ligands.

HY-161415

BCL-xL/BCL-2 ligand 1	2941091-91-2
BCL-xL/BCL-2 ligand 1 (compound 72-1) is a BCL-xL and BCL-2 protein ligand. BCL-xL/BCL-2 ligand 1 can be connected to the E3 ligase by a linker to form PROTACs (HY-161410).

HY-W584525

VH032-NH-CO-CH2-NHBoc	2010986-19-1
VH032-NH-CO-CH2-NHBoc is a Boc-modified VH032 (HY-120217) that acts as a ligand for VHL to recruit von Hippel-Lindau (VHL) proteins. VH032-NH-CO-CH2-NHBoc will remove the Boc protection under acidic conditions, and connect with the target protein ligand through a linker to form a PROTAC molecule, which is a key intermediate for the synthesis of PROTAC based on VHL ligand.

HY-168226

E3 ligase Ligand 34	2931870-73-2
E3 ligase Ligand 34 is the E3 ligase ligand part of PROTAC SMARCA2/4-degrader-35 (HY-168225) and can be utilized in the synthesis of PROTACs.

HY-159973

Me-SJ46411
Me-SJ46411 is an E3 ubiquitin ligase ligand, which can be used for the synthesis of PROTAC molecules. For example, Me-SJ46411 combined with PROTAC linker Boc-Piperazine-OH (HY-20797) and target protein ligand (+)-JQ-1 (HY-13030) can be used to synthesize the selective BRD3 PROTAC degrader SJ46420 (HY-168635)..

HY-178874

E3 ligase Ligand 75	3063924-16-0
E3 ligase Ligand 75 is an E3 ligase ligand. E3 ligase Ligand 75 can be used for synthesis PROTAC K-Ras Degrader-7 (HY-178873).

HY-169390

OICR-8268-acrylic acid
OICR-8268-acrylic acid is a ligand for E3 ubiquitin ligase. OICR-8268-acrylic acid can be connected to the ligand for protein by a linker to form OICR41114 (HY-169389). OICR41114 can be used in anti-cancer research.

HY-170348

(S)-(S,R,S,R)-AHPC-Me-N3	2958620-43-2
(S)-(S,R,S,R)-AHPC-Me-N3 serves as the E3 ligase ligand for PROTAC SMARCA2 degrader-32 (HY-170343) and can be used in the synthesis of PROTACs.

HY-P11493

ALAPYIP	1260529-82-5
ALAPYIP is a ligand for E3 ligase. ALAPYIP recruits the VHL-E3 ubiquitin ligase. ALAPYIP can be used for the synthesis of FPP29 (HY-P11228).

HY-163951

(S,R,S)-AHPC-Ac	2361116-63-2
(S,R,S)-AHPC-Ac is a ligand for E3 ubiquitinase. (S,R,S)-AHPC-Ac can be used to synthesize PROTAC SMARCA2/4-degrader-22 (HY-163875).

HY-162855

E3 ligase Ligand 33	3023410-43-4
E3 ligase Ligand 33 (56-9B) is a ligand for E3 ubiquitin ligase. E3 ligase Ligand 33 can be used in anti-cancer research.

HY-163932

(S,R,S)-AHPC-O-CF3	2641373-92-2
(S,R,S)-AHPC-O-CF3 is a ligand for E3 ubiquitinase. (S,R,S)-AHPC-O-CF3 can be used to synthesize PROTAC SMARCA2/4-degrader-20 (HY-163873).

HY-101763B

(S,R,S)-AHPC dihydrochloride	2137142-47-1
(S,R,S)-AHPC (VH032-NH2) dihydrochloride is the VH032-based VHL ligand used in the recruitment of the von Hippel-Lindau (VHL) protein. (S,R,S)-AHPC dihydrochloride can be connected to the ligand for protein (e.g., BCR-ABL1) by a linker to form PROTACs (e.g., GMB-475). GMB-475 induces the degradation of BCR-ABL1 with an IC₅₀ of 1.11 μM in Ba/F3 cells.

HY-168232

E3 ligase Ligand 35
E3 ligase Ligand 35 serves as the E3 ligase ligand for PROTAC SMARCA2 degrader-27 (HY-168229).

HY-168646

SJ46411-Br
SJ46411-Br is one of CRL2^KLHDC2 targeting Ligands for E3 Ligase. SJ46411-Br can bind to KLHDC2 to form a complex to promote cooperative homologous selective ternary complex formation. SJ46411-Br can be coupled to BET ligand JQ1 (HY-13030) through PROTAC linker to synthesize corresponding PROTACs.

HY-401613

E3 ligase Ligand 43	2821795-71-3
E3 ligase Ligand 43 serves as the E3 ubiquitin ligase ligand for ACBI3 (HY-157228). E3 ligase Ligand 43 can be utilized for the synthesis of PROTACs.

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