Purine metabolism

Purine metabolism refers to the metabolic pathways to synthesize and break down purines that are present in many organisms.

Biosynthesis

Purines are biologically synthesized as nucleotides and in particular as ribotides, i.e. bases attached to ribose 5-phosphate. Both adenine and guanine are derived from the nucleotide inosine monophosphate (IMP), which is the first compound in the pathway to have a completely formed purine ring system.

IMP

Inosine monophosphate is synthesized on a pre-existing ribose-phosphate through a complex pathway (as shown in the figure on the right). The source of the

10-formyltetrahydrofolate, and a carbon atom from bicarbonate

(1). Formyl groups build carbon-2 and carbon-8 in the purine ring system, which are the ones acting as bridges between two nitrogen atoms.

A key regulatory step is the production of 5-phospho-α-D-ribosyl 1-pyrophosphate (

inorganic phosphate

and inactivated by purine ribonucleotides. It is not the committed step to purine synthesis because PRPP is also used in pyrimidine synthesis and salvage pathways.

The first committed step is the reaction of PRPP,

glutamate, and pyrophosphate - catalyzed by amidophosphoribosyltransferase, which is activated by PRPP and inhibited by AMP, GMP and IMP

.

PRPP + L-Glutamine + H₂O → PRA + L-Glutamate + PPi

In the second step react PRA, glycine and ATP to create GAR, ADP, and pyrophosphate - catalyzed by phosphoribosylamine—glycine ligase (GAR synthetase). Due to the chemical lability of PRA, which has a half-life of 38 seconds at PH 7.5 and 37 °C, researchers have suggested that the compound is channeled from amidophosphoribosyltransferase to GAR synthetase in vivo.^[1]

PRA + Glycine + ATP → GAR + ADP + Pi

The third is catalyzed by phosphoribosylglycinamide formyltransferase.

GAR + fTHF → fGAR + THF

The fourth is catalyzed by phosphoribosylformylglycinamidine synthase.

fGAR + L-Glutamine + ATP →

fGAM

+ L-Glutamate + ADP + Pi

The fifth is catalyzed by AIR synthetase (FGAM cyclase).

fGAM + ATP → AIR + ADP + Pi + H₂O

The sixth is catalyzed by phosphoribosylaminoimidazole carboxylase.

AIR + CO₂ →

CAIR + 2H+

The seventh is catalyzed by phosphoribosylaminoimidazolesuccinocarboxamide synthase.

CAIR + L-Aspartate + ATP → SAICAR + ADP + Pi

The eight is catalyzed by adenylosuccinate lyase.

SAICAR → AICAR + Fumarate

The products AICAR and fumarate move on to two different pathways. AICAR serves as the reactant for the ninth step, while fumarate is transported to the citric acid cycle which can then skip the carbon dioxide evolution steps to produce malate. The conversion of fumarate to malate is catalyzed by fumarase. In this way, fumarate connects purine synthesis to the citric acid cycle.^[2]

The ninth is catalyzed by phosphoribosylaminoimidazolecarboxamide formyltransferase.

AICAR + fTHF → FAICAR + THF

The last step is catalyzed by Inosine monophosphate synthase.

FAICAR → IMP + H₂O

In eukaryotes the second, third, and fifth step are catalyzed by trifunctional purine biosynthetic protein adenosine-3, which is encoded by the GART gene.

Both ninth and tenth step are accomplished by a single protein named Bifunctional purine biosynthesis protein PURH, encoded by the ATIC gene.

GMP

IMP into XMP

GMP

GMP reductase converts GMP back into IMP

AMP

adenylosuccinate synthase converts IMP to adenylosuccinate
adenylosuccinate lyase converts adenylosuccinate into AMP
AMP deaminase converts AMP back into IMP

Degradation

Purines are metabolised by several enzymes:

Guanine

A nuclease frees the nucleotide
A nucleotidase creates guanosine
Purine nucleoside phosphorylase converts guanosine to guanine
Guanase converts guanine to xanthine

oxidation of xanthine to uric acid

Adenine

A nuclease frees the nucleotide
- A nucleotidase creates adenosine, then adenosine deaminase creates inosine
- Alternatively, AMP deaminase creates inosinic acid, then a nucleotidase creates inosine
Purine nucleoside phosphorylase acts upon inosine to create hypoxanthine
Xanthine oxidase catalyzes the biotransformation of hypoxanthine to xanthine
Xanthine oxidase acts upon xanthine to create uric acid

Regulations of purine nucleotide biosynthesis

The formation of 5'-phosphoribosylamine from glutamine and PRPP catalysed by PRPP amino transferase is the regulation point for purine synthesis. The enzyme is an allosteric enzyme, so it can be converted from IMP, GMP and AMP in high concentration binds the enzyme to exerts inhibition while PRPP is in large amount binds to the enzyme which causes activation. So IMP, GMP and AMP are inhibitors while PRPP is an activator. Between the formation of 5'-phosphoribosyl, aminoimidazole and IMP, there is no known regulation step.

Salvage

Purines from turnover of cellular nucleic acids (or from food) can also be salvaged and reused in new nucleotides.

The enzyme adenine phosphoribosyltransferase (APRT) salvages adenine.
The enzyme hypoxanthine-guanine phosphoribosyltransferase (HGPRT) salvages guanine and hypoxanthine.^[3] (Genetic deficiency of HGPRT causes Lesch–Nyhan syndrome.)

Disorders

When a defective gene causes gaps to appear in the metabolic recycling process for purines and pyrimidines, these chemicals are not metabolised properly, and adults or children can suffer from any one of twenty-eight hereditary disorders, possibly some more as yet unknown. Symptoms can include gout, anaemia, epilepsy, delayed development, deafness, compulsive self-biting, kidney failure or stones, or loss of immunity.

Purine metabolism can have imbalances that can arise from harmful nucleotide triphosphates incorporating into DNA and RNA which further lead to genetic disturbances and mutations, and as a result, give rise to several types of diseases. Some of the diseases are:

Severe immunodeficiency by loss of adenosine deaminase.
Hyperuricemia and Lesch–Nyhan syndrome by the loss of hypoxanthine-guanine phosphoribosyltransferase.
Different types of cancer by an increase in the activities of enzymes like IMP dehydrogenase.^[4]

Pharmacotherapy

Modulation of purine metabolism has pharmacotherapeutic value.

Purine synthesis inhibitors inhibit the proliferation of cells, especially

organ transplantation, autoimmune disease such as rheumatoid arthritis or inflammatory bowel disease such as Crohn's disease and ulcerative colitis

.

Mycophenolate mofetil is an immunosuppressant drug used to prevent rejection in organ transplantation; it inhibits purine synthesis by blocking inosine monophosphate dehydrogenase (IMPDH).^[5]

folic acid (it is an inhibitor of the dihydrofolate reductase

).

Allopurinol is a drug that inhibits the enzyme xanthine oxidoreductase and, thus, lowers the level of uric acid in the body. This may be useful in the treatment of gout, which is a disease caused by excess uric acid, forming crystals in joints.

Prebiotic synthesis of purine ribonucleosides

In order to understand how life arose, knowledge is required of the chemical pathways that permit formation of the key building blocks of life under plausible prebiotic conditions. Nam et al.^[6] demonstrated the direct condensation of purine and pyrimidine nucleobases with ribose to give ribonucleosides in aqueous microdroplets, a key step leading to RNA formation. Also, a plausible prebiotic process for synthesizing purine ribonucleosides was presented by Becker et al.^[7]

Purine biosynthesis in the three domains of life

Organisms in all three domains of life, eukaryotes, bacteria and archaea, are able to carry out de novo biosynthesis of purines. This ability reflects the essentiality of purines for life. The biochemical pathway of synthesis is very similar in eukaryotes and bacterial species, but is more variable among archaeal species.^[8] A nearly complete, or complete, set of genes required for purine biosynthesis was determined to be present in 58 of the 65 archaeal species studied.^[8] However, also identified were seven archaeal species with entirely, or nearly entirely, absent purine encoding genes. Apparently the archaeal species unable to synthesize purines are able to acquire exogenous purines for growth.,^[8] and are thus similar to purine mutants of eukaryotes, e.g. purine mutants of the Ascomycete fungus Neurospora crassa,^[9] that also require exogenous purines for growth.

References

PMID 8626510
.

OCLC 914290655.{{cite book}}: CS1 maint: location missing publisher (link
)

PMID 26616453
.

PMID 22308425
.

^ "Mycophenolate Monograph for Professionals". Drugs.com. Archived from the original on 21 April 2020. Retrieved 28 October 2019.

^ Nam I, Nam HG, Zare RN. Abiotic synthesis of purine and pyrimidine ribonucleosides in aqueous microdroplets. Proc Natl Acad Sci U S A. 2018 Jan 2;115(1):36-40. doi: 10.1073/pnas.1718559115. Epub 2017 Dec 18. PMID 29255025; PMCID: PMC5776833

^ Becker S, Thoma I, Deutsch A, Gehrke T, Mayer P, Zipse H, Carell T. A high-yielding, strictly regioselective prebiotic purine nucleoside formation pathway. Science. 2016 May 13;352(6287):833-6. doi: 10.1126/science.aad2808. PMID 27174989.

^ ^a ^b ^c Brown AM, Hoopes SL, White RH, Sarisky CA. Purine biosynthesis in archaea: variations on a theme. Biol Direct. 2011 Dec 14;6:63. doi: 10.1186/1745-6150-6-63. PMID 22168471; PMCID: PMC3261824

^ Bernstein, H. Imidazole compounds accumulated by purine mutants of Neurospora crassa J. Gen. Microbiol. 5:41-46 (1961)

External links

The Medical Biochemistry Page

Purine metabolism - Reference pathway

PUMPA: Purine Metabolic Patients’ Association

v
t
e
Metabolism, catabolism, anabolism
General

Metabolic pathway

Metabolic network

Primary nutritional groups

Aerobic respiration

Glycolysis → Pyruvate decarboxylation → Citric acid cycle → Oxidative phosphorylation (electron transport chain + ATP synthase)

Anaerobic respiration

Electron acceptors other than oxygen

Fermentation

Glycolysis → Substrate-level phosphorylation
ABE

Ethanol

Lactic acid

Specific
paths
Protein metabolism

Protein synthesis

Catabolism (protein→peptide→amino acid)

Amino acid

Amino acid synthesis

Amino acid degradation (amino acid→pyruvate, acetyl CoA, or TCA intermediate)

Urea cycle

Nucleotide
metabolism

Purine metabolism

Nucleotide salvage

Pyrimidine metabolism

Purine nucleotide cycle

Carbohydrate metabolism
(carbohydrate catabolism
and anabolism)
Human

Glycolysis ⇄ Gluconeogenesis

Glycogenolysis ⇄ Glycogenesis

Pentose phosphate pathway

Fructolysis
Polyol pathway

Galactolysis
Leloir pathway

Glycosylation
N-linked

O-linked

Nonhuman

Photosynthesis

Anoxygenic photosynthesis

Chemosynthesis

Carbon fixation

DeLey-Doudoroff pathway

Entner-Doudoroff pathway

Xylose metabolism

Radiotrophism

Lipid metabolism
(lipolysis, lipogenesis)
Fatty acid metabolism

Fatty acid degradation (Beta oxidation)

Fatty acid synthesis

Other

Steroid metabolism

Sphingolipid metabolism

Eicosanoid metabolism

Ketosis

Reverse cholesterol transport

Other

Metal metabolism
Iron metabolism

Ethanol metabolism

Phospagen system (ATP-PCr)

v
t
e

Metabolism: amino acid metabolism

nucleotide enzymes

Purine metabolism
Anabolism
R5P→IMP:

Ribose-phosphate diphosphokinase

Amidophosphoribosyltransferase

Phosphoribosylglycinamide formyltransferase

AIR synthetase (FGAM cyclase)

Phosphoribosylaminoimidazole carboxylase

Phosphoribosylaminoimidazolesuccinocarboxamide synthase

IMP synthase

IMP→AMP:

Adenylosuccinate synthase

Adenylosuccinate lyase

reverse
AMP deaminase

IMP→GMP:

IMP dehydrogenase

GMP synthase

reverse
GMP reductase

Nucleotide salvage

Hypoxanthine-guanine phosphoribosyltransferase

Adenine phosphoribosyltransferase

Catabolism

Adenosine deaminase

Purine nucleoside phosphorylase

Guanine deaminase

Xanthine oxidase

Urate oxidase

Pyrimidine metabolism
Anabolism

CAD

Carbamoyl phosphate synthase II

Aspartate carbamoyltransferase

Dihydroorotase

Dihydroorotate dehydrogenase

Uridine monophosphate synthetase

CTP synthetase

Catabolism

Dihydropyrimidine dehydrogenase

Dihydropyrimidinase/DPYS

Beta-ureidopropionase/UPB1

Deoxyribonucleotides

Ribonucleotide reductase

Nucleoside-diphosphate kinase

DCMP deaminase

Thymidylate synthase

Dihydrofolate reductase

v
t
e
Nucleotide metabolic intermediates
purine
metabolism
anabolism
R5P→IMP:

Ribose 5-phosphate (R5P)

Phosphoribosyl pyrophosphate (PRPP)

Phosphoribosylamine (PRA)

Glycineamide ribonucleotide (GAR)

Phosphoribosyl-N-formylglycineamide (FGAR)

5′-Phosphoribosylformylglycinamidine (FGAM)

5-Aminoimidazole ribotide (AIR)

5′-Phosphoribosyl-4-carboxy-5-aminoimidazole (CAIR)

Phosphoribosylaminoimidazolesuccinocarboxamide (SAICAR)

AICA ribonucleotide (AICAR)

5-Formamidoimidazole-4-carboxamide ribotide (FAICAR)

IMP→AMP:
Adenylosuccinate
IMP→GMP:
Xanthosine monophosphate
catabolism

5-Hydroxyisourate

Hypoxanthine

Uric acid

Xanthine

pyrimidine
metabolism
anabolism

Carbamoyl aspartic acid

Carbamoyl phosphate

4,5-Dihydroorotic acid

Orotic acid

Orotidine 5'-monophosphate

Uridine monophosphate

catabolism
uracil:

β-Alanine

Dihydrouracil

3-Ureidopropionic acid

thymine:

3-Aminoisobutyric acid

Dihydrothymine

β-Ureidoisobutyric acid

Inborn error of purine–pyrimidine metabolism
Purine metabolism
Anabolism

Adenylosuccinate lyase deficiency

Adenosine Monophosphate Deaminase Deficiency type 1

Nucleotide salvage

Lesch–Nyhan syndrome/Hyperuricemia

Adenine phosphoribosyltransferase deficiency

Catabolism

Adenosine deaminase deficiency

Purine nucleoside phosphorylase deficiency

Xanthinuria

Gout

Mitochondrial neurogastrointestinal encephalopathy syndrome

Pyrimidine metabolism
Anabolism

Orotic aciduria

Miller syndrome

Catabolism

Dihydropyrimidine dehydrogenase deficiency

P0 (adenine
)

Agonists: 8-Aminoadenine

Adenine

P1
(adenosine)

Agonists: 2-(1-Hexynyl)-N-methyladenosine

2-Cl-IB-MECA

2'-MeCCPA

4'-O-β-D-Glucosyl-9-O-(6''-deoxysaccharosyl)olivil

5'-N-ethylcarboxamidoadenosine

Adenosine

ADP

AMP

Apadenoson

ATL-146e

ATP

BAY 60–6583

Binodenoson

Capadenoson

CCPA

CGS-21680

CP-532,903

Evodenoson

GR 79236

LUF-5835

LUF-5845

N⁶-Cyclopentyladenosine

Namodenoson

Neladenoson dalanate

Piclidenoson

Regadenoson

SDZ WAG 994

Selodenoson

Sonedenoson

Tecadenoson

UK-432,097

Antagonists: 7-Methylxanthine

8-Chlorotheophylline

8-Phenyl-1,3-dipropylxanthine

8-Phenyltheophylline

Acefylline

Aminophylline

ATL-444

Bamifylline

Cafedrine

Caffeine

Caffeine citrate

Cartazolate

CGH-2466

CGS-15943

Choline theophyllinate

Ciforadenant

CPX

CVT-6883

Dimethazan

DMPX

DPCPX

Dyphylline

Enprofylline

Etazolate

Fenethylline

IBMX

Isovaleric acid

Istradefylline

KF-26777

MRE3008F20

MRS-1220

MRS-1334

MRS-1706

MRS-1754

MRS-3777

Paraxanthine

Pentoxifylline

Preladenant

Propentofylline

Proxyphylline

PSB-10

PSB-11

PSB-36

PSB-603

PSB-788

PSB-1115

Reversine

Rolofylline

SCH-442,416

SCH-58261

Theacrine

Theobromine

Theodrenaline

Theophylline

Tozadenant

Tracazolate

VUF-5574

ZM-241,385

P2
(nucleotide)
P2X
(ATPTooltip Adenosine triphosphate)

Agonists: 2-Me-SATP

α,β-Me-ATP

Adenosine

ADP

AMP

Ap4A

Ap5A

ATP

ATPγS

BzATP

Cibacron blue

CTP

D-β,γ-Me-ATP

GTP

HT-AMP

Ivermectin

L-β,γ-Me-ATP

MRS-2219

PAPET-ATP

UTP

Zinc

Antagonists: 5-BDBD

A-317491

A-438079

A-740003

A-804598

A-839977

AF-353

AZ-10606120

AZ-11645373

BBG

Calcium

Calmidazolium

Chelerythrine

Copper

Emodin (Rheum officinale)

Evans blue

Gefapixant

GW-791343

HMA

Ip5I

isoPPADS

JNJ-47965567

KN-04

KN-62

Magnesium

MRS-2159

NF-023

NF-110

NF-157

NF-279

NF-449

Opiranserin (VVZ-149)

Oxidized-ATP

Phenol Red

Phenolphthalein

PPADS

PPNDS

PSB-12062

Radix puerariae
)

Purotoxin 1

RB-2

Ro 0437626

Ro 51

RO-3

Ligusticum wallichii
)

Suramin

TC-P 262

Ligusticum wallichii
)

TNP-ATP

Zinc

P2Y

Agonists: 2-Me-SADP

2-Me-SATP

2-Thio-UTP

5-Br-UDP

5-OMe-UDP

α,β-Me-ATP

Adenosine

ADP

ADPβS

Ap3A

AR-C 67085MX

ATP

ATPγS

CTP

dATP

Denufosol

Diquafosol

IDP

ITP

INS-365

INS-37217

MRS-2365

MRS-2690

MRS-2693

MRS-2768

MRS-2957

MRS-4062

NF-546

PAPET-ATP

PSB-0474

PSB-1114

UDP

UDPβS

UDP-galactose

UDP-glucose

UDP-N-acetylglucosamine

Up3U

UTP

UTPγS

Antagonists: 2-Me-SAMP

A3P5PS

AMPαS

Ap4A

AR-C 66096

AR-C 67085MX

AR-C 69931MX

AR-C 118925XX

ATP

BzATP

C1330-7

Cangrelor

Clopidogrel

Elinogrel

Ip5I

MRS-2179

MRS-2211

MRS-2279

MRS-2395

MRS-2500

MRS-2578

NF-157

NF-340

PIT

PPADS

Prasugrel

PSB-0739

RB-2

Regrelor

Suramin

Ticagrelor

Ticlopidine

UDP

CNTs
Tooltip Concentrative nucleoside transporters

6-Hydroxy-7-methoxyflavone

Adenosine

dMeThPmR

Estradiol

KGO-2142

KGO-2173

MeThPmR

Phloridzin

Progesterone

ENTs
Tooltip Equilibrative nucleoside transporters

Barbiturates

Benzodiazepines

Cilostazol

Dilazep

Dipyridamole

Estradiol

Ethanol

Hexobendine

NBMPR

Pentoxifylline

Progesterone

Propentofylline

PMATTooltip Plasma membrane monoamine transporter

Decynium-22

Enzyme
(inhibitors)
XOTooltip Xanthine oxidase

Allopurinol

Amflutizole

Benzbromarone

Caffeic acid

Cinnamaldehyde

Cinnamomum osmophloeum

Febuxostat

Myo-inositol

Kaempferol

Myricetin

Niraxostat

Oxipurinol

Phytic acid

Pistacia integerrima

Propolis

Quercetin

Tisopurine

Topiroxostat

Others

Aminopterin

Azathioprine

Methotrexate

Mycophenolic acid

Pemetrexed

Pralatrexate

Many others

Others

Precursors: Adenine

Adenosine

AMP

ADP

ATP

Cytosine

Cytidine

CMP

CDP

CTP

Guanine

Guanosine

GMP

GDP

GTP

Hypoxanthine

Inosine

IMP

IDP

ITP

Ribose

Uracil

Uridine

UMP

UDP

UTP

Others: Chrysophanol (rhubarb)

See also: Receptor/signaling modulators

Retrieved from "https://en.wikipedia.org/w/index.php?title=Purine_metabolism&oldid=1143059350"

[1] PMID 8626510
.

[2] OCLC 914290655.{{cite book}}: CS1 maint: location missing publisher (link
)

[pmid26616453-3] PMID 26616453
.

[4] PMID 22308425
.

[5] "Mycophenolate Monograph for Professionals". Drugs.com. Archived from the original on 21 April 2020. Retrieved 28 October 2019.

[6] Nam I, Nam HG, Zare RN. Abiotic synthesis of purine and pyrimidine ribonucleosides in aqueous microdroplets. Proc Natl Acad Sci U S A. 2018 Jan 2;115(1):36-40. doi: 10.1073/pnas.1718559115. Epub 2017 Dec 18. PMID 29255025; PMCID: PMC5776833

[7] Becker S, Thoma I, Deutsch A, Gehrke T, Mayer P, Zipse H, Carell T. A high-yielding, strictly regioselective prebiotic purine nucleoside formation pathway. Science. 2016 May 13;352(6287):833-6. doi: 10.1126/science.aad2808. PMID 27174989.

[Brown2011-8] Brown AM, Hoopes SL, White RH, Sarisky CA. Purine biosynthesis in archaea: variations on a theme. Biol Direct. 2011 Dec 14;6:63. doi: 10.1186/1745-6150-6-63. PMID 22168471; PMCID: PMC3261824

[9] Bernstein, H. Imidazole compounds accumulated by purine mutants of Neurospora crassa J. Gen. Microbiol. 5:41-46 (1961)

[1]

[2]

[3]

[4]

[5]

[6]

[7]

[8]

[9]