CYP17A1
CYTOCHROME P-450 (CYP450)

Author: Gianpiero Pescarmona
Date: 03/08/2013

Description

DEFINITION

CYP17A1 is the gene that encodes for the enzyme Cytochrome P450 17A1 ( or steroid 17-alpha-monooxygenase, or 17α-hydroxylase/17,20 lyase/17,20 desmolase) . It is found in the zona reticularis of the adrenal cortex and it localizes to the endoplasmic reticulum. It has both 17alpha-hydroxylase and 17,20-lyase activities, and is a key enzyme in the steroidogenic pathway that produces progestins, mineralocorticoids, glucocorticoids, androgens, and estrogens.

THE GENE

Database	Link
Wikigenes	CYP17A1
GeneCards	CYP17A1
Your Favorite Gene Sigma	CYP17A1

CHEMICAL STRUCTURE AND IMAGES

When relevant for the function

Primary structure
Secondary structure
Tertiary structure
**"PDB":http://www.rcsb.org/pdb/home/home.do;jsessionid=8EA7FAAF417856601ED3CA796882DDB9
Quaternary structure

Protein Aminoacids Percentage
The Protein Aminoacids Percentage gives useful information on the local environment and the metabolic status of the cell (starvation, lack of essential AA, hypoxia)

Protein Aminoacids Percentage (Width 700 px)

SYNTHESIS AND TURNOVER

mRNA synthesis

!{width:56px;height:20px}http://flipper.diff.org/static/files/1011/Quertle-70.gif!CYP17A1 expression induction

protein synthesis

post-translational modifications
degradation

CELLULAR FUNCTIONS

cellular localization,
biological function

Enzymes

Database	Link
BRENDA - The Comprehensive Enzyme Information System	"URL":
KEGG Pathways	"URL":
Human Metabolome Database	"URL":

Cell signaling and Ligand transport
Structural proteins

REGULATION

Mechanism of action of anti-aging DHEA-S and the replacement of DHEA-S. 2002

The mechanism of dissociation of cortisol and DHEA synthesis in aging depends on another regulator of 17,20-lyase of cytochrome P450c17 such as cytochrome P450 reductase.

NADPH P450 oxidoreductase: Structure, function, and pathology of diseases 2013

Cytochrome P450 oxidoreductase (POR) is an enzyme that is essential for multiple metabolic processes, chiefly among them are reactions catalyzed by cytochrome P450 proteins for metabolism of steroid hormones, drugs and xenobiotics. Mutations in POR cause a complex set of disorders that often resemble defects in steroid metabolizing enzymes 17α-hydroxylase, 21-hydroxylase and aromatase. Since our initial reports of POR mutations in 2004, more than 200 different mutations and polymorphisms in POR gene have been identified. Several missense variations in POR have been tested for their effect on activities of multiple steroid and drug metabolizing P450 proteins. Mutations in POR may have variable effects on different P450 partner proteins depending on the location of the mutation. The POR mutations that disrupt the binding of co-factors have negative impact on all partner proteins, while mutations causing subtle structural changes may lead to altered interaction with specific partner proteins and the overall effect may be different for each partner. This review summarizes the recent discoveries related to mutations and polymorphisms in POR and discusses these mutations in the context of historical developments in the discovery and characterization of POR as an electron transfer protein. The review is focused on the structural, enzymatic and clinical implications of the mutations linked to newly identified disorders in humans, now categorized as POR deficiency.

DIAGNOSTIC USE

Comments

2013-08-03T14:19:37 - Gianpiero Pescarmona

A clinical/translational perspective: Can a developmental hormone play a role in the treatment of traumatic brain injury? 2913

Cytochrome b5: Novel roles in steroidogenesis, 2012

Proposed function of cyt-b5 in CYP17A1 catalysis. (I) NADPH transfers two electrons to POR. (II) FMN domain of POR rotates to dock with the redox-partner binding site on CYP17A1, resulting in the 17α-hydroxylation of the steroid substrate. (III) cyt-b5 acts as an allosteric effector to optimize the geometry required for the 17,20-lyase reaction. Reproduced from (Auchus et al., 1998).