MYF5

MYF5
Identifiers
Gene ontology
Molecular function	DNA binding; sequence-specific DNA binding; protein dimerization activity; DNA-binding transcription activator activity, RNA polymerase II-specific; RNA polymerase II cis-regulatory region sequence-specific DNA binding; E-box binding; protein binding; protein heterodimerization activity; transcription factor activity, RNA polymerase II distal enhancer sequence-specific binding; DNA-binding transcription factor activity, RNA polymerase II-specific;
Cellular component	nucleoplasm; RNA polymerase II transcription regulator complex; nucleus;
Biological process	somitogenesis; embryonic skeletal system morphogenesis; cell differentiation; regulation of transcription, DNA-templated; muscle organ morphogenesis; ossification; positive regulation of muscle cell differentiation; regulation of transcription by RNA polymerase II; muscle cell fate commitment; muscle organ development; extracellular matrix organization; transcription by RNA polymerase II; positive regulation of skeletal muscle fiber development; transcription, DNA-templated; regulation of cell-matrix adhesion; multicellular organism development; positive regulation of myoblast fusion; positive regulation of myoblast differentiation; muscle tissue morphogenesis; skeletal muscle cell differentiation; camera-type eye development; skeletal muscle tissue development; cartilage condensation; positive regulation of transcription by RNA polymerase II;
	Sources:Amigo / QuickGO

Ensembl


ENSG00000111049


ENSMUSG00000000435

UniProt


P13349


P24699

RefSeq (mRNA)


NM_005593


NM_008656

RefSeq (protein)


NP_005584


NP_032682

Location (UCSC)

Chr 12: 80.72 – 80.72 Mb

Chr 10: 107.32 – 107.32 Mb

PubMed search

^[3]

^[4]

Wikidata

View/Edit Human

View/Edit Mouse

Myogenic factor 5 is a protein that in humans is encoded by the MYF5 gene. ^[5] It is a

MRF4 (Myf6).^[6] This transcription factor is the earliest of all MRFs to be expressed in the embryo, where it is only markedly expressed for a few days (specifically around 8 days post-somite formation and lasting until day 14 post-somite in mice).^[7] It functions during that time to commit myogenic precursor cells to become skeletal muscle. In fact, its expression in proliferating myoblasts has led to its classification as a determination factor. Furthermore, Myf5 is a master regulator of muscle development, possessing the ability to induce a muscle phenotype upon its forced expression in fibroblastic cells.^[8]

Expression

Myf5 is expressed in the dermomyotome of the early somites, pushing the myogenic precursors to undergo determination and differentiate into myoblasts.[7] Specifically, it is first seen in the dorsomedial portion of the dermomyotome, which develops into the epaxial myotome.^[7] Although it is expressed in both the epaxial (to become muscles of the back) and hypaxial (body wall and limb muscles) portions of the myotome, it is regulated differently in these tissue lines, providing part of their alternative differentiation. Most notably, while Myf5 is activated by Sonic hedgehog in the epaxial lineage,^[9] it is instead directly activated by the transcription factor Pax3 in hypaxial cells.^[10] The limb myogenic precursors (derived from the hypaxial myotome) do not begin expressing Myf5 or any MRFs, in fact, until after migration to the limb buds.^[11] Myf5 is also expressed in non-somitic paraxial mesoderm that forms muscles of the head, at least in zebrafish.^[12]

While the product of this gene is capable of directing cells towards the skeletal muscle lineage, it is not absolutely required for this process. Numerous studies have shown redundancy with two other MRFs, MyoD and MRF4. The absence of all three of these factors results in a phenotype with no skeletal muscle.^[13] These studies were performed after it was shown that Myf5 knockouts had no clear abnormality in their skeletal muscle.^[14] The high redundancy of this system shows how crucial the development of skeletal muscle is to the viability of the fetus. Some evidence shows that Myf5 and MyoD are responsible for the development of separate muscle lineages, and are not expressed concurrently in the same cell.^[15] Specifically, while Myf5 plays a large role in the initiation of epaxial development, MyoD directs the initiation of hypaxial development, and these separate lineages can compensate for the absence of one or the other. This has led some to claim that they are not indeed redundant, though this depends on the definition of the word. Still, the existence of these separate “MyoD-dependent” and “Myf5-dependent” subpopulations has been disputed, with some claiming that these MRFs are indeed coexpressed in muscle progenitor cells.^[10] This debate is ongoing.

Although Myf5 is mainly associated with myogenesis, it is expressed in other tissues, as well. Firstly, it is expressed in brown adipose precursors. However, its expression is limited to brown and not white adipose precursors, providing part of the developmental separation between these two lineages.^[16] Furthermore, Myf5 is expressed in portions of the neural tube (that go on to form neurons) a few days after it is seen in the somites. This expression is eventually repressed to prevent extraneous muscle formation.^[17] Although the specific roles and dependency of Myf5 in adipogenesis and neurogenesis have remained to be explored, these findings show that Myf5 may play roles outside of myogenesis. Myf5 also has an indirect role controlling proximal rib development. Although Myf5 knockouts have normal skeletal muscle, they die due to abnormalities in their proximal ribs that make it difficult to breathe.^[15]

Despite only being present for a few days during embryonic development, Myf5 is still expressed in certain adult cells. As one of the key cell markers of satellite cells (the stem cell pool for skeletal muscles), it plays an important role in the regeneration of adult muscle.^[18] Specifically, it allows a brief pulse of proliferation of these satellite cells in response to injury. Differentiation begins (regulated by other genes) after this initial proliferation. In fact, if Myf5 is not downregulated, differentiation does not occur.^[19]

In zebrafish, Myf5 is the first MRF expressed in embryonic myogenesis and is required for adult viability, even though larval muscle forms normally. As no muscle is formed in Myf5;Myod double mutant zebrafish, Myf5 cooperates with Myod to promote myogenesis.^[20]

Regulation

The regulation of Myf5 is dictated by a large number of enhancer elements that allow a complex system of regulation. Although most events throughout myogenesis that involve Myf5 are controlled through the interaction of multiple enhancers, there is one important early enhancer that initiates expression. Termed the early epaxial enhancer, its activation provides the "go" signal for expression of Myf5 in the epaxial dermomyotome, where it is first seen.^[21] Sonic hedgehog from the neural tube acts at this enhancer to activate it.^[9] Following that, the chromosome contains different enhancers for regulation of Myf5 expression in the hypaxial region, cranial region, limbs, etc.^[21] This early expression of Myf5 in the epaxial dermamyotome is involved with the very formation of myotome, but nothing beyond that. After its initial expression, other enhancer elements dictate where and how long it is expressed. It remains clear that each population of myogenic progenitor cells (for different locations in the embryo) is regulated by a different set of enhancers.^[22]

Clinical significance

As for its clinical significance, the aberration of this transcription factor provides part of the mechanism for how hypoxia (lack of oxygen) can influence muscle development. Hypoxia has the ability to impede muscle differentiation in part by inhibiting the expression of Myf5 (as well as other MRFs). This prevents the muscle precursors from becoming post-mitotic muscle fibers. Although hypoxia is a teratogen, this inhibition of expression is reversible, therefore it remains unclear if there is a connection between hypoxia and birth defects in the fetus.^[23]

References

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000111049 - Ensembl, May 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000000435 - Ensembl, May 2017
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "Entrez Gene: Myogenic factor 5". Retrieved 2013-08-19.
S2CID 22496065
.

^
PMID 1652425
.

PMID 2721498
.

^
PMID 11782449
.

^
S2CID 18747744
.

PMID 8290594
.

PMID 17007832
.

S2CID 4413512
.

S2CID 27322641
.

^
PMID 18331721
.

PMID 17360536
.

PMID 8575308
.

PMID 11121437
.

S2CID 28853682
.

PMID 21798255
.

^
PMID 10934019
.

PMID 12223413
.

PMID 14754880
.

Further reading

Krauss RS, Cole F, Gaio U, Takaesu G, Zhang W, Kang JS (June 2005). "Close encounters: regulation of vertebrate skeletal myogenesis by cell-cell contact". Journal of Cell Science. 118 (Pt 11): 2355–62.
PMID 15923648
.

Summerbell D, Halai C, Rigby PW (September 2002). "Expression of the myogenic regulatory factor Mrf4 precedes or is contemporaneous with that of Myf5 in the somitic bud". Mechanisms of Development. 117 (1–2): 331–5.
S2CID 5947462
.

Langlands K, Yin X, Anand G, Prochownik EV (August 1997). "Differential interactions of Id proteins with basic-helix-loop-helix transcription factors". The Journal of Biological Chemistry. 272 (32): 19785–93.
PMID 9242638
.

Dimicoli-Salazar S, Bulle F, Yacia A, Massé JM, Fichelson S, Vigon I (November 2011). "Efficient in vitro myogenic reprogramming of human primary mesenchymal stem cells and endothelial cells by Myf5". Biology of the Cell. 103 (11): 531–42.
S2CID 23776022
.

Cupelli L, Renault B, Leblanc-Straceski J, Banks A, Ward D, Kucherlapati RS, Krauter K (1996). "Assignment of the human myogenic factors 5 and 6 (MYF5, MYF6) gene cluster to 12q21 by in situ hybridization and physical mapping of the locus between D12S350 and D12S106". Cytogenetics and Cell Genetics. 72 (2–3): 250–1.
PMID 8978788
.

Ansseau E, Laoudj-Chenivesse D, Marcowycz A, Tassin A, Vanderplanck C, Sauvage S, Barro M, Mahieu I, Leroy A, Leclercq I, Mainfroid V, Figlewicz D, Mouly V, Butler-Browne G, Belayew A, Coppée F (2009). Callaerts P (ed.). "DUX4c is up-regulated in FSHD. It induces the MYF5 protein and human myoblast proliferation". PLOS ONE. 4 (10): e7482.
PMID 19829708
.

Winter B, Kautzner I, Issinger OG, Arnold HH (December 1997). "Two putative protein kinase CK2 phosphorylation sites are important for Myf-5 activity". Biological Chemistry. 378 (12): 1445–56.
S2CID 6218391
.

Chen CM, Kraut N, Groudine M, Weintraub H (September 1996). "I-mf, a novel myogenic repressor, interacts with members of the MyoD family". Cell. 86 (5): 731–41.
S2CID 16252710
.

Braun T, Buschhausen-Denker G, Bober E, Tannich E, Arnold HH (March 1989). "A novel human muscle factor related to but distinct from MyoD1 induces myogenic conversion in 10T1/2 fibroblasts". The EMBO Journal. 8 (3): 701–9.
PMID 2721498
.

v
t
e
Transcription factors and intracellular receptors
(1) Basic domains
(1.1) Basic leucine zipper (bZIP)

Activating transcription factor
AATF

1

2

3

4

5

6

7

AP-1
c-Fos

FOSB

FOSL1

FOSL2

JDP2

c-Jun

JUNB

JunD

BACH
1

2

BATF

BLZF1

C/EBP

α

β

γ

δ

ε

ζ

CREB
1

3

L1

CREM

DBP

DDIT3

GABPA

GCN4

HLF

MAF
B

F

G

K

NFE
2

L1

L2

L3

NFIL3

NRL

NRF
1

2

3

XBP1

(1.2) Basic helix-loop-helix (
bHLH
)
Group A

AS-C
ASCL1

ASCL2

ATOH1

HAND
1

2

MESP2

Myogenic regulatory factors
MyoD

Myogenin

MYF5

MYF6

NeuroD
1

2

Neurogenins
1

2

3

OLIG
1

2

Paraxis
TCF15

Scleraxis

SLC
LYL1

TAL
1

2

Twist

Group B

FIGLA

Myc
c-Myc

l-Myc

n-Myc

MXD4

TCF4

Group C
bHLH-PAS

AhR

AHRR

ARNT
ARNTL

ARNTL2

CLOCK

HIF
1A

EPAS1

3A

NPAS
1

2

3

PER
1

2

3

Period

SIM
1

2

Group D

BHLH
2

3

9

Pho4

ID
1

2

3

4

Group E

HES
1

2

3

4

5

6

7

HEY
1

2

L

Group F
bHLH-COE

EBF1

(1.3) bHLH-ZIP

AP-4

MAX
MXD1

MXD3

MITF

MNT

MLX

MLXIPL

MXI1

Myc

SREBP
1

2

USF1

(1.4) NF-1

NFI
A

B

C

X

SMAD
R-SMAD
1

2

3

5

9

I-SMAD
6

7

4)

(1.5) RF-X

RFX
1

2

3

4

5

6

ANK

(1.6) Basic helix-span-helix (bHSH)

AP-2
α

β

γ

δ

ε

(2) Zinc finger DNA-binding domains
(2.1) Nuclear receptor (Cys₄)
subfamily 1

Thyroid hormone
α

β

CAR

FXR

LXR
α

β

PPAR
α

β/δ

γ

PXR

RAR
α

β

γ

ROR
α

β

γ

Rev-ErbA

α

β

VDR

subfamily 2

COUP-TF
(I

II

Ear-2

HNF4
α

γ

PNR

RXR
α

β

γ

Testicular receptor
2

4

TLX

subfamily 3

Steroid hormone
Androgen

Estrogen
α

β

Glucocorticoid

Mineralocorticoid

Progesterone

Estrogen related
α

β

γ

subfamily 4

NUR

NGFIB

NOR1

NURR1

subfamily 5

LRH-1

SF1

subfamily 6

GCNF

subfamily 0

DAX1

SHP

(2.2) Other Cys₄

GATA
1

2

3

4

5

6

MTA
1

2

3

TRPS1

(2.3) Cys₂His₂

General transcription factors
TFIIA

TFIIB

TFIID

TFIIE
1

2

TFIIF

1

2
TFIIH

1

2

4

2I

3A

3C1

3C2

ATBF1

BCL
6

11A

11B

CTCF

E4F1

EGR
1

2

3

4

ERV3

GFI1

GLI family
1

2

3

REST

S1

S2

YY1

HIC
1

2

HIVEP
1

2

3

IKZF
1

2

3

ILF
2

3

Sp/KLF family
KLF
1

2

3

4

5

6

7

8

9

10

11

12

13

14

15

17

SP
1

2

4

7

8

MTF1

MYT1

OSR1

PRDM9

SALL
1

2

3

4

TSHZ3

WT1

Zbtb7
7A

7B

ZBTB
11

16

17

20

21

32

33

40

zinc finger
3

7

9

10

19

22

24

33B

34

35

41

43

44

51

74

143

146

148

165

202

217

219

238

239

259

267

268

281

300

318

330

346

350

365

366

384

423

451

452

471

593

638

644

649

655

804A

(2.4) Cys₆

HIVEP1

(2.5) Alternating composition

AIRE

DIDO1

GRLF1

ING
1

2

4

JARID
1A

1B

1C

1D

2

JMJD1B

(2.6) WRKY

WRKY

(3)
Homeodomain
Antennapedia
ANTP class
protoHOX
Hox-like

ParaHox
Gsx
1

2

Xlox

PDX1

Cdx
1

2

4

extended Hox: Evx1

Evx2

MEOX1

MEOX2

Homeobox
A1

A2

A3

A4

A5

A7

A9

A10

A11

A13

B1

B2

B3

B4

B5

B6

B7

B8

B9

B13

C4

C5

C6

C8

C9

C10

C11

C12

C13

D1

D3

D4

D8

D9

D10

D11

D12

D13

GBX1

GBX2

MNX1

metaHOX
NK-like

BARHL1

BARHL2

BARX1

BARX2

BSX

DBX
1

2

DLX
1

2

3

4

5

6

EMX
1

2

EN
1

2

HHEX

HLX

LBX1

LBX2

MSX
1

2

NANOG

NKX
2-1

2-2

2-3

2-5

3-1

3-2

HMX1

HMX2

HMX3

6-1

6-2

NATO

TLX1

TLX2

TLX3

VAX1

VAX2

other

ARX

CRX

CUTL1

FHL
1

2

3

HESX1

HOPX

LMX
1A

1B

NOBOX

TALE
IRX
1

2

3

4

5

6

MKX

MEIS
1

2

PBX
1

2

3

PKNOX
1

2

SIX
1

2

3

4

5

PHF
1

3

6

8

10

16

17

20

21A

POU domain
PIT-1

BRN-3: A

B

C

Octamer transcription factor: 1

2

3/4

6

7

11

SATB2

ZEB
1

2

(3.2) Paired box

PAX
1

2

3

4

5

6

7

8

9

PRRX
1

2

PROP1

PHOX
2A

2B

RAX

SHOX

SHOX2

VSX1

VSX2

Bicoid

GSC

BICD2

OTX
1

2

PITX
1

2

3

(3.3) Fork head / winged helix

E2F
1

2

3

4

5

FOX proteins
A1

A2

A3

B1

B2

C1

C2

D1

D2

D3

D4

D4L1

D4L3

D4L4

D4L5

D4L6

E1

E3

F1

F2

G1

H1

I1

I2

I3

J1

J2

J3

K1

K2

L1

L2

M1

N1

N2

N3

N4

O1

O3

O4

O6

P1

P2

P3

P4

Q1

R1

R2

S1

(3.4) Heat shock factors

HSF
1

2

4

(3.5) Tryptophan clusters

ELF
2

4

5

EGF

ELK
1

3

4

ERF

ETS
1

2

ERG

SPIB

ETV
1

4

5

6

FLI1

Interferon regulatory factors
1

2

3

4

5

6

7

8

MYB

MYBL2

(3.6) TEA domain

transcriptional enhancer factor
1

2

3

4

(4) β-Scaffold factors with minor groove contacts
(4.1) Rel homology region

NF-κB
NFKB1

NFKB2

REL

RELA

RELB

NFAT
C1

C2

C3

C4

5

(4.2) STAT

STAT
1

2

3

4

5

6

(4.3) p53-like

p53 p63 p73 family
p53

TP63

p73

TBX
1

2

3

5

19

21

22

TBR1

TBR2

TFT

MYRF

(4.4) MADS box

Mef2
A

B

C

D

SRF

(4.6) TATA-binding proteins

TBP

TBPL1

(4.7) High-mobility group

BBX

HMGB
1

2

3

4

HMGN
1

2

3

4

HNF
1A

1B

SOX
1

2

3

4

5

6

8

9

10

11

12

13

14

15

18

21

SRY

SSRP1

TCF/LEF
TCF
1

3

4

LEF1

TOX
1

2

3

4

(4.9) Grainyhead

TFCP2

(4.10) Cold-shock domain

CSDA

YBX1

(4.11) Runt

CBF
CBFA2T2

CBFA2T3

RUNX1

RUNX2

RUNX3

RUNX1T1

(0) Other transcription factors
(0.2) HMGI(Y)

HMGA
1

2

HBP1

(0.3) Pocket domain

Rb

RBL1

RBL2

(0.5) AP-2/EREBP-related factors

Apetala 2

EREBP

B3

(0.6) Miscellaneous

ARID
1A

1B

2

3A

3B

4A

CAP

IFI
16

35

MLL

2

3

T1

MNDA

NFY
A

B

C

Rho/Sigma

see also transcription factor/coregulator deficiencies

Retrieved from "https://en.wikipedia.org/w/index.php?title=MYF5&oldid=1094225880"

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000111049 - Ensembl, May 2017

[refGRCm38Ensembl-2] GRCm38: Ensembl release 89: ENSMUSG00000000435 - Ensembl, May 2017

[3] "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[4] "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[entrez-5] "Entrez Gene: Myogenic factor 5". Retrieved 2013-08-19.

[pmid10733231-6] S2CID 22496065
.

[:0-7] 
PMID 1652425
.

[8] PMID 2721498
.

[:1-9] 
PMID 11782449
.

[:2-10] 
S2CID 18747744
.

[11] PMID 8290594
.

[12] PMID 17007832
.

[13] S2CID 4413512
.

[14] S2CID 27322641
.

[:3-15] 
PMID 18331721
.

[16] PMID 17360536
.

[17] PMID 8575308
.

[18] PMID 11121437
.

[19] S2CID 28853682
.

[20] PMID 21798255
.

[:4-21] 
PMID 10934019
.

[22] PMID 12223413
.

[23] PMID 14754880
.

[3]

[4]

[5]

[6]

[7]

[8]

[9]

[10]

[11]

[12]

[13]

[14]

[15]

[16]

[17]

[18]

[19]

[20]

[21]

[22]

[23]