Drug Information

Drug (ID: DG01695) and It's Reported Resistant Information

Name	Cisplatin/Pictilisib
Synonyms	Cisplatin/Pictilisib Click to Show/Hide
Target	.	NOUNIPROTAC	[1]

Type(s) of Resistant Mechanism of This Drug

UAPP: Unusual Activation of Pro-survival Pathway

Drug Resistance Data Categorized by Their Corresponding Diseases

ICD-02: Benign/in-situ/malignant neoplasm

Click to Show/Hide the Resistance Disease of This Class

Bladder cancer [ICD-11: 2C94]

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Drug Sensitivity Data Categorized by Their Corresponding Mechanisms
Unusual Activation of Pro-survival Pathway (UAPP)			Click to Show/Hide
Key Molecule: PI3-kinase alpha (PIK3CA)				[1]
Molecule Alteration	Missense mutation		p.H1047R (c.3140A>G)	Molecule Info
Sensitive Disease	Bladder cancer [ICD-11: 2C94.0]			Disease Info
Experimental Note	Identified from the Human Clinical Data
Cell Pathway Regulation	MEK/ERK signaling pathway		Inhibition	hsa04011
In Vitro Model	5637 cells	Bladder	Homo sapiens (Human)	CVCL_0126
	J82 cells	Bladder	Homo sapiens (Human)	CVCL_0359
	RT4 cells	Bladder	Homo sapiens (Human)	CVCL_0036
	T24 cells	Bladder	Homo sapiens (Human)	CVCL_0554
	TCCSuP cells	Bladder	Homo sapiens (Human)	CVCL_1738
In Vivo Model	NSG mouse PDX model			Mus musculus
Experiment for Drug Resistance	MTS assay; FACS assay
Mechanism Description	Pictilisib activated the compensatory MEK/ERK pathways that likely contributed to pictilisib resistance, which was reversed by co-treatment with the RAF inhibitor sorafenib. RNA-sequencing of tumors resistant to treatment suggested that LSP1 down-regulation correlated with drug resistance.

References

Ref 1	The Phosphatidylinositol 3-Kinase Pathway as a Potential Therapeutic Target in Bladder CancerClin Cancer Res. 2017 Nov 1;23(21):6580-6591. doi: 10.1158/1078-0432.CCR-17-0033. Epub 2017 Aug 14.

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