fbpx
Wikipedia

Enediyne

January 01, 1970

Enediynes are organic compounds containing two triple bonds and one double bond.

The enediyne functional group
Calicheamicin: An antitumor antibiotic featuring an enediyne unit

Enediynes are most notable for their limited use as antitumor antibiotics (known as enediyne anticancer antibiotics).[1] They are efficient at inducing apoptosis in cells, but cannot differentiate cancerous cells from healthy cells. Consequently, research is being conducted to increase the specificity of enediyne toxicity.

Structure and reactivity edit

A nine- or ten-membered ring containing a double bond between two triple bonds is termed the warhead of the enediyne. In this state, the warhead is inactive. Enediynes are triggered into a chemically active state via Bergman or Myers-Saito cyclization. The triggering mechanism can be attributed to an intramolecular nucleophilic attack initiated by one of the variable regions of the molecule. Triggering can also occur via attack by an external nucleophile.[citation needed]

Bergman cyclization restructures the enediyne ring into two smaller rings. One electron from each of the enediyne triple bonds is pushed to the adjacent single bonds, generating two new double bonds. Meanwhile, another pair of electrons (one from each alkyne) is used form a new covalent bond. The resulting formation is a 1,4-benzenoid diradical fused to a ring composed of the leftover atoms from the original enediyne.

 
Electron pushing that occurs during Bergman cyclization in a generic enediyne molecule. A 1,4-benzenoid diradical fused to another ring is the result.

Some enediynes have an epoxide group attached to their ring, making Bergman cyclization unfavorable due to steric hindrance. For Bergman cyclization to occur, the epoxide must be removed.

Myers-Saito cyclization is another triggering mechanism by which an enediyne warhead becomes a diradical. This mechanism requires the alkene of the enediyne to be part of a diene with a double bond in a variable group. A nucleophile will attack the double bond in the variable region, causing a chain reaction of electron pushing. Ultimately, one of the triple bonds of the enediyne is converted to a cumulene.[2] The cumulene and the remaining alkyne donate one electron each to form a new covalent bond.

 
A generic enediyne molecule is pictured above. During Myers-Saito cyclization, electrons pushing begins at the diene and generates an unstable cumulene. This cumulene and the nearby alkyne donate one electron to split the enediyne ring into two fused rings.

The diradicals generated by Bergman and Myers-Saito cyclization are highly reactive.[citation needed]

Mechanism of action edit

 
Abstraction of hydrogen from either the C1, C4, or C5 position of the sugar phosphate backbone of DNA by a reactive 1,4-benzenoid

The cyclization of the enediyne functional group creates a transient reactive 1,4-benzenoid diradical that acts as a nucleophile and attacks electrophiles in order to achieve a more stable form. In biological systems, once the diradical is positioned in the minor groove of double-stranded DNA, it abstracts two hydrogen atoms from the sugars opposite strands at either the C1, C4, or C5 positions.[3] The DNA radicals that form can then cause interstrand crosslinks or react with O2, leading to double- or single-stranded DNA cleavage.[4]

Biosynthesis edit

Members of the enediyne family all share a unique enediyne core that is the cause of their potent cytotoxicity.[5] The enediyne cores are derived from linear, probably polyketide, precursors that consist of seven or eight head-to-tail coupled acetate units. Enediyne assembly involves a highly conserved, iterative type I polyketide synthase (PKS) pathway[6] Sequencing of enediyne gene clusters has confirmed the polyketide origin of the enediyne core, and elucidated the biosynthetic pathways and mechanisms of enediynes.[7]

Differences in the biosynthetic pathways of enediynes are due to the different origins of the -yne carbons as well as differences in isotope incorporation patterns. More differentiation comes from the attachment of various functional groups at different positions to the enediyne warheads during their maturation stage. These moieties can be either aromatic or sugars and define sequence specificity of DNA binding as well as the physical properties of the enediyne chromophores.[5]

Due to the cytotoxicity of the enediyne chromophores, their biosynthesis is tightly regulated, although the regulatory mechanisms are still largely unclear. Organisms that produce enediynes have been shown to protect themselves with a self-resistance mechanism that uses a self-sacrificing protein. Notably, some microbes use CalC to sequester calicheamicin so that the reactive diradical abstracts hydrogens from a glycine inside of the protein instead of from DNA.[5]

Classes edit

There are fourteen naturally occurring enediynes.[6] The other existing classes of enediynes have been synthesized in the lab.

Enediynes have been split into two sub-families: those with nine members in the core enediyne ring and those with ten-membered rings.[citation needed]

Nine-membered rings (chromoproteins) edit

The nine-membered enediynes are also referred to as chromoproteins because they have an attached protein as a variable group. This protein is necessary for transport and stabilization of the enediyne group.[8]

Neocarzinostatin edit

Neocarzinostatin is a natural product of Streptomyces carzinostaticus. It forms an apoprotein with a 113-amino acid polypeptide which can cleave histone protein H1.[9] Neocarzinostatin is an example of an enediyne that undergoes triggering via Myers-Saito cyclization. An analog of neocarzinostatin, SMANCS, has been approved for use in Japan as an antitumor drug for liver cancer.[10]

C-1027 edit

Also known as lidamycin, C-1027 is one of the most potent antitumor enediynes. C-1027 was first isolated from Streptomyces globisporus in a soil sample taken from the Qian-Jiang District of China. Unlike most enediynes, C-1027 does not undergo a triggering process to become an activated 1,4-benzenoid diradical.[11] C-1027 has demonstrated potential efficacy against hypoxic tumors.[4]

Ten-membered rings edit

Calicheamicins edit

The calicheamicins are a sub-family of enediynes that were isolated from Micromonospora echinospora calichensis.[12] All calicheamicin family members demonstrate potent antimicrobial activity against Gram-positive and Gram-negative organisms.[12] Calicheamicin γ1 exhibited significant antitumor activity against leukemia and melanoma cells in vivo.[12] The calicheamicins are notably similar in structure to the esperamicins.

Esperamicins edit

The esperamicins are a sub-family of enediynes that are considered among the most potent antitumor antibiotics discovered.[13] First isolated in Actinomadura verrucosospora, members of the esperamicin family include esperamicin A1, A1b, A2, A3, A4, B1, B2, and X. Esperamicin X is an inactive esperamicin naturally produced by A. verrucosospora.[13] Compounds with thiol groups induce triggering among the esperamicins.[14]

Dynemicins edit

The dynemicins are a sub-family of enediynes whose members are organic compounds generated in Micromonospora chersina.[8] Dynemicin A was the first member of this sub-family to be discovered. It was isolated from M. chersina in a soil sample taken from the state of Gujarat in India.[15] Dynemicins are violet in color because they contain anthraquinone as a variable group attached to the enediyne core.[8] Dynemycins have demonstrated strong antitumor activity against leukemia and melanoma cells.[16]

Golfomycin A edit

Golfomycin A is a synthetic enediyne molecule designed in an attempt to create a more easily manufactured antitumor antibiotic.[17] DNA strand-scission induced by golfomycin A is pH dependent.[17] Preliminary in vitro studies have demonstrated that golfomycin A can reduce carcinomas in bladder cells.[17]

See also edit

References edit

  1. ^ Nicolaou KC, Smith AL, Yue EW (July 1993). "Chemistry and biology of natural and designed enediynes". Proceedings of the National Academy of Sciences of the United States of America. 90 (13): 5881–8. Bibcode:1993PNAS...90.5881N. doi:10.1073/pnas.90.13.5881. PMC 46830. PMID 8327459.
  2. ^ "Bergman Cyclization". www.organic-chemistry.org. Retrieved 2018-05-05.
  3. ^ Smith AL, Nicolaou KC (May 1996). "The enediyne antibiotics". Journal of Medicinal Chemistry. 39 (11): 2103–17. doi:10.1021/jm9600398. PMID 8667354.
  4. ^ a b Chen Y, Yin M, Horsman GP, Shen B (March 2011). "Improvement of the enediyne antitumor antibiotic C-1027 production by manipulating its biosynthetic pathway regulation in Streptomyces globisporus". Journal of Natural Products. 74 (3): 420–4. doi:10.1021/np100825y. PMC 3064734. PMID 21250756.
  5. ^ a b c Liang ZX (April 2010). "Complexity and simplicity in the biosynthesis of enediyne natural products". Natural Product Reports. 27 (4): 499–528. doi:10.1039/b908165h. PMID 20336235.
  6. ^ a b Shen B, Hindra, Yan X, Huang T, Ge H, Yang D, Teng Q, Rudolf JD, Lohman JR (January 2015). "Enediynes: Exploration of microbial genomics to discover new anticancer drug leads". Bioorganic & Medicinal Chemistry Letters. 25 (1): 9–15. doi:10.1016/j.bmcl.2014.11.019. PMC 4480864. PMID 25434000.
  7. ^ Van Lanen SG, Shen B (2008). "Biosynthesis of enediyne antitumor antibiotics". Current Topics in Medicinal Chemistry. 8 (6): 448–59. doi:10.2174/156802608783955656. PMC 3108100. PMID 18397168.
  8. ^ a b c Gao Q, Thorson JS (May 2008). "The biosynthetic genes encoding for the production of the dynemicin enediyne core in Micromonospora chersina ATCC53710". FEMS Microbiology Letters. 282 (1): 105–14. doi:10.1111/j.1574-6968.2008.01112.x. PMC 5591436. PMID 18328078.
  9. ^ Heyd B, Lerat G, Adjadj E, Minard P, Desmadril M (April 2000). "Reinvestigation of the proteolytic activity of neocarzinostatin". Journal of Bacteriology. 182 (7): 1812–8. doi:10.1128/jb.182.7.1812-1818.2000. PMC 101862. PMID 10714984.
  10. ^ Maeda H (March 2001). "SMANCS and polymer-conjugated macromolecular drugs: advantages in cancer chemotherapy". Advanced Drug Delivery Reviews. 46 (1–3): 169–85. doi:10.1016/s0169-409x(00)00134-4. PMID 11259839.
  11. ^ Xu YJ, Zhen YS, Goldberg IH (May 1994). "C1027 chromophore, a potent new enediyne antitumor antibiotic, induces sequence-specific double-strand DNA cleavage". Biochemistry. 33 (19): 5947–54. doi:10.1021/bi00185a036. PMID 8180224.
  12. ^ a b c Maiese WM, Lechevalier MP, Lechevalier HA, Korshalla J, Kuck N, Fantini A, Wildey MJ, Thomas J, Greenstein M (April 1989). "Calicheamicins, a novel family of antitumor antibiotics: taxonomy, fermentation and biological properties". The Journal of Antibiotics. 42 (4): 558–63. doi:10.7164/antibiotics.42.558. PMID 2722671.
  13. ^ a b Golik J, Clardy J, Dubay G, Groenewold G, Kawaguchi H, Konishi M, Krishnan B, Ohkuma H, Saitoh K (May 1987). "Esperamicins, a novel class of potent antitumor antibiotics. 2. Structure of esperamicin X". Journal of the American Chemical Society. 109 (11): 3461–3462. doi:10.1021/ja00245a048. ISSN 0002-7863.
  14. ^ Sugiura Y, Uesawa Y, Takahashi Y, Kuwahara J, Golik J, Doyle TW (October 1989). "Nucleotide-specific cleavage and minor-groove interaction of DNA with esperamicin antitumor antibiotics". Proceedings of the National Academy of Sciences of the United States of America. 86 (20): 7672–6. Bibcode:1989PNAS...86.7672S. doi:10.1073/pnas.86.20.7672. PMC 298132. PMID 2813351.
  15. ^ Konishi M, Ohkuma H, Matsumoto K, Tsuno T, Kamei H, Miyaki T, Oki T, Kawaguchi H, VanDuyne GD, Clardy J (September 1989). "Dynemicin A, a novel antibiotic with the anthraquinone and 1,5-diyn-3-ene subunit". The Journal of Antibiotics. 42 (9): 1449–52. doi:10.7164/antibiotics.42.1449. PMID 2793600.
  16. ^ Unno R, Michishita H, Inagaki H, Suzuki Y, Baba Y, Jomori T, Nishikawa T, Isobe M (May 1997). "Synthesis and antitumor activity of water-soluble enediyne compounds related to dynemicin A". Bioorganic & Medicinal Chemistry. 5 (5): 987–99. doi:10.1016/s0968-0896(97)00037-0. PMID 9208107.
  17. ^ a b c Nicolaou KC, Skokotas G, Furuya S, Suemune H, Nicolaou DC (September 1990). "Golfomycin A, a Novel Designed Molecule with DNA-Cleaving Properties and Antitumor Activity". Angewandte Chemie International Edition in English. 29 (9): 1064–1067. doi:10.1002/anie.199010641. ISSN 0570-0833.

January 01, 1970
enediyne, organic, compounds, containing, triple, bonds, double, bond, enediyne, functional, groupcalicheamicin, antitumor, antibiotic, featuring, enediyne, unit, most, notable, their, limited, antitumor, antibiotics, known, enediyne, anticancer, antibiotics, . Enediynes are organic compounds containing two triple bonds and one double bond The enediyne functional groupCalicheamicin An antitumor antibiotic featuring an enediyne unit Enediynes are most notable for their limited use as antitumor antibiotics known as enediyne anticancer antibiotics 1 They are efficient at inducing apoptosis in cells but cannot differentiate cancerous cells from healthy cells Consequently research is being conducted to increase the specificity of enediyne toxicity Contents 1 Structure and reactivity 2 Mechanism of action 3 Biosynthesis 4 Classes 4 1 Nine membered rings chromoproteins 4 1 1 Neocarzinostatin 4 1 2 C 1027 4 2 Ten membered rings 4 2 1 Calicheamicins 4 2 2 Esperamicins 4 2 3 Dynemicins 4 2 4 Golfomycin A 5 See also 6 ReferencesStructure and reactivity editA nine or ten membered ring containing a double bond between two triple bonds is termed the warhead of the enediyne In this state the warhead is inactive Enediynes are triggered into a chemically active state via Bergman or Myers Saito cyclization The triggering mechanism can be attributed to an intramolecular nucleophilic attack initiated by one of the variable regions of the molecule Triggering can also occur via attack by an external nucleophile citation needed Bergman cyclization restructures the enediyne ring into two smaller rings One electron from each of the enediyne triple bonds is pushed to the adjacent single bonds generating two new double bonds Meanwhile another pair of electrons one from each alkyne is used form a new covalent bond The resulting formation is a 1 4 benzenoid diradical fused to a ring composed of the leftover atoms from the original enediyne nbsp Electron pushing that occurs during Bergman cyclization in a generic enediyne molecule A 1 4 benzenoid diradical fused to another ring is the result Some enediynes have an epoxide group attached to their ring making Bergman cyclization unfavorable due to steric hindrance For Bergman cyclization to occur the epoxide must be removed Myers Saito cyclization is another triggering mechanism by which an enediyne warhead becomes a diradical This mechanism requires the alkene of the enediyne to be part of a diene with a double bond in a variable group A nucleophile will attack the double bond in the variable region causing a chain reaction of electron pushing Ultimately one of the triple bonds of the enediyne is converted to a cumulene 2 The cumulene and the remaining alkyne donate one electron each to form a new covalent bond nbsp A generic enediyne molecule is pictured above During Myers Saito cyclization electrons pushing begins at the diene and generates an unstable cumulene This cumulene and the nearby alkyne donate one electron to split the enediyne ring into two fused rings The diradicals generated by Bergman and Myers Saito cyclization are highly reactive citation needed Mechanism of action edit nbsp Abstraction of hydrogen from either the C1 C4 or C5 position of the sugar phosphate backbone of DNA by a reactive 1 4 benzenoid The cyclization of the enediyne functional group creates a transient reactive 1 4 benzenoid diradical that acts as a nucleophile and attacks electrophiles in order to achieve a more stable form In biological systems once the diradical is positioned in the minor groove of double stranded DNA it abstracts two hydrogen atoms from the sugars opposite strands at either the C1 C4 or C5 positions 3 The DNA radicals that form can then cause interstrand crosslinks or react with O2 leading to double or single stranded DNA cleavage 4 Biosynthesis editMembers of the enediyne family all share a unique enediyne core that is the cause of their potent cytotoxicity 5 The enediyne cores are derived from linear probably polyketide precursors that consist of seven or eight head to tail coupled acetate units Enediyne assembly involves a highly conserved iterative type I polyketide synthase PKS pathway 6 Sequencing of enediyne gene clusters has confirmed the polyketide origin of the enediyne core and elucidated the biosynthetic pathways and mechanisms of enediynes 7 Differences in the biosynthetic pathways of enediynes are due to the different origins of the yne carbons as well as differences in isotope incorporation patterns More differentiation comes from the attachment of various functional groups at different positions to the enediyne warheads during their maturation stage These moieties can be either aromatic or sugars and define sequence specificity of DNA binding as well as the physical properties of the enediyne chromophores 5 Due to the cytotoxicity of the enediyne chromophores their biosynthesis is tightly regulated although the regulatory mechanisms are still largely unclear Organisms that produce enediynes have been shown to protect themselves with a self resistance mechanism that uses a self sacrificing protein Notably some microbes use CalC to sequester calicheamicin so that the reactive diradical abstracts hydrogens from a glycine inside of the protein instead of from DNA 5 Classes editThere are fourteen naturally occurring enediynes 6 The other existing classes of enediynes have been synthesized in the lab Enediynes have been split into two sub families those with nine members in the core enediyne ring and those with ten membered rings citation needed Nine membered rings chromoproteins edit The nine membered enediynes are also referred to as chromoproteins because they have an attached protein as a variable group This protein is necessary for transport and stabilization of the enediyne group 8 Neocarzinostatin edit Neocarzinostatin is a natural product of Streptomyces carzinostaticus It forms an apoprotein with a 113 amino acid polypeptide which can cleave histone protein H1 9 Neocarzinostatin is an example of an enediyne that undergoes triggering via Myers Saito cyclization An analog of neocarzinostatin SMANCS has been approved for use in Japan as an antitumor drug for liver cancer 10 C 1027 edit Also known as lidamycin C 1027 is one of the most potent antitumor enediynes C 1027 was first isolated from Streptomyces globisporus in a soil sample taken from the Qian Jiang District of China Unlike most enediynes C 1027 does not undergo a triggering process to become an activated 1 4 benzenoid diradical 11 C 1027 has demonstrated potential efficacy against hypoxic tumors 4 Ten membered rings edit Calicheamicins editThe calicheamicins are a sub family of enediynes that were isolated from Micromonospora echinospora calichensis 12 All calicheamicin family members demonstrate potent antimicrobial activity against Gram positive and Gram negative organisms 12 Calicheamicin g1 exhibited significant antitumor activity against leukemia and melanoma cells in vivo 12 The calicheamicins are notably similar in structure to the esperamicins Esperamicins edit The esperamicins are a sub family of enediynes that are considered among the most potent antitumor antibiotics discovered 13 First isolated in Actinomadura verrucosospora members of the esperamicin family include esperamicin A1 A1b A2 A3 A4 B1 B2 and X Esperamicin X is an inactive esperamicin naturally produced by A verrucosospora 13 Compounds with thiol groups induce triggering among the esperamicins 14 Dynemicins edit The dynemicins are a sub family of enediynes whose members are organic compounds generated in Micromonospora chersina 8 Dynemicin A was the first member of this sub family to be discovered It was isolated from M chersina in a soil sample taken from the state of Gujarat in India 15 Dynemicins are violet in color because they contain anthraquinone as a variable group attached to the enediyne core 8 Dynemycins have demonstrated strong antitumor activity against leukemia and melanoma cells 16 Golfomycin A edit Golfomycin A is a synthetic enediyne molecule designed in an attempt to create a more easily manufactured antitumor antibiotic 17 DNA strand scission induced by golfomycin A is pH dependent 17 Preliminary in vitro studies have demonstrated that golfomycin A can reduce carcinomas in bladder cells 17 See also editEnyne metathesis Enyne PolyyneReferences edit Nicolaou KC Smith AL Yue EW July 1993 Chemistry and biology of natural and designed enediynes Proceedings of the National Academy of Sciences of the United States of America 90 13 5881 8 Bibcode 1993PNAS 90 5881N doi 10 1073 pnas 90 13 5881 PMC 46830 PMID 8327459 Bergman Cyclization www organic chemistry org Retrieved 2018 05 05 Smith AL Nicolaou KC May 1996 The enediyne antibiotics Journal of Medicinal Chemistry 39 11 2103 17 doi 10 1021 jm9600398 PMID 8667354 a b Chen Y Yin M Horsman GP Shen B March 2011 Improvement of the enediyne antitumor antibiotic C 1027 production by manipulating its biosynthetic pathway regulation in Streptomyces globisporus Journal of Natural Products 74 3 420 4 doi 10 1021 np100825y PMC 3064734 PMID 21250756 a b c Liang ZX April 2010 Complexity and simplicity in the biosynthesis of enediyne natural products Natural Product Reports 27 4 499 528 doi 10 1039 b908165h PMID 20336235 a b Shen B Hindra Yan X Huang T Ge H Yang D Teng Q Rudolf JD Lohman JR January 2015 Enediynes Exploration of microbial genomics to discover new anticancer drug leads Bioorganic amp Medicinal Chemistry Letters 25 1 9 15 doi 10 1016 j bmcl 2014 11 019 PMC 4480864 PMID 25434000 Van Lanen SG Shen B 2008 Biosynthesis of enediyne antitumor antibiotics Current Topics in Medicinal Chemistry 8 6 448 59 doi 10 2174 156802608783955656 PMC 3108100 PMID 18397168 a b c Gao Q Thorson JS May 2008 The biosynthetic genes encoding for the production of the dynemicin enediyne core in Micromonospora chersina ATCC53710 FEMS Microbiology Letters 282 1 105 14 doi 10 1111 j 1574 6968 2008 01112 x PMC 5591436 PMID 18328078 Heyd B Lerat G Adjadj E Minard P Desmadril M April 2000 Reinvestigation of the proteolytic activity of neocarzinostatin Journal of Bacteriology 182 7 1812 8 doi 10 1128 jb 182 7 1812 1818 2000 PMC 101862 PMID 10714984 Maeda H March 2001 SMANCS and polymer conjugated macromolecular drugs advantages in cancer chemotherapy Advanced Drug Delivery Reviews 46 1 3 169 85 doi 10 1016 s0169 409x 00 00134 4 PMID 11259839 Xu YJ Zhen YS Goldberg IH May 1994 C1027 chromophore a potent new enediyne antitumor antibiotic induces sequence specific double strand DNA cleavage Biochemistry 33 19 5947 54 doi 10 1021 bi00185a036 PMID 8180224 a b c Maiese WM Lechevalier MP Lechevalier HA Korshalla J Kuck N Fantini A Wildey MJ Thomas J Greenstein M April 1989 Calicheamicins a novel family of antitumor antibiotics taxonomy fermentation and biological properties The Journal of Antibiotics 42 4 558 63 doi 10 7164 antibiotics 42 558 PMID 2722671 a b Golik J Clardy J Dubay G Groenewold G Kawaguchi H Konishi M Krishnan B Ohkuma H Saitoh K May 1987 Esperamicins a novel class of potent antitumor antibiotics 2 Structure of esperamicin X Journal of the American Chemical Society 109 11 3461 3462 doi 10 1021 ja00245a048 ISSN 0002 7863 Sugiura Y Uesawa Y Takahashi Y Kuwahara J Golik J Doyle TW October 1989 Nucleotide specific cleavage and minor groove interaction of DNA with esperamicin antitumor antibiotics Proceedings of the National Academy of Sciences of the United States of America 86 20 7672 6 Bibcode 1989PNAS 86 7672S doi 10 1073 pnas 86 20 7672 PMC 298132 PMID 2813351 Konishi M Ohkuma H Matsumoto K Tsuno T Kamei H Miyaki T Oki T Kawaguchi H VanDuyne GD Clardy J September 1989 Dynemicin A a novel antibiotic with the anthraquinone and 1 5 diyn 3 ene subunit The Journal of Antibiotics 42 9 1449 52 doi 10 7164 antibiotics 42 1449 PMID 2793600 Unno R Michishita H Inagaki H Suzuki Y Baba Y Jomori T Nishikawa T Isobe M May 1997 Synthesis and antitumor activity of water soluble enediyne compounds related to dynemicin A Bioorganic amp Medicinal Chemistry 5 5 987 99 doi 10 1016 s0968 0896 97 00037 0 PMID 9208107 a b c Nicolaou KC Skokotas G Furuya S Suemune H Nicolaou DC September 1990 Golfomycin A a Novel Designed Molecule with DNA Cleaving Properties and Antitumor Activity Angewandte Chemie International Edition in English 29 9 1064 1067 doi 10 1002 anie 199010641 ISSN 0570 0833 Retrieved from https en wikipedia org w index php title Enediyne amp oldid 1184032035, wikipedia, wiki, book, books, library,

article

, read, download, free, free download, mp3, video, mp4, 3gp, jpg, jpeg, gif, png, picture, music, song, movie, book, game, games.