Igfals MGI Mouse Gene Detail - MGI:107973 - insulin-like growth factor binding protein, acid labile subunit

About Help FAQ

Igfals Gene Detail

Symbol

Igfals
Name

insulin-like growth factor binding protein, acid labile subunit
Synonyms

Albs, ALS

Feature Type

protein coding gene
IDs

MGI:107973
NCBI Gene: 16005
Alliance

gene page
Transcription Start Sites

5 TSS
Candidate for QTL

4 QTL

more

Sequence Map

Chr17:25096818-25100985 bp, + strand
From NCBI annotation of GRCm39
View this region in JBrowse
Genome Browsers

Ensembl | UCSC | NCBI

Genetic Map

Chromosome 17, 12.53 cM, cytoband A2-A3
Mapping Data

4 experiments

more

SNPs within 2kb

177 from dbSNP Build 142
Strain Annotations

18

For selected strains:

Strain	Gene Model ID	Feature Type	Coordinates	Select Strains
C57BL/6J	MGI_C57BL6J_107973	protein coding gene	Chr17:25084971-25100985 (+)
129S1/SvImJ	MGP_129S1SvImJ_G0023326	protein coding gene	Chr17:23904217-23907455 (+)
A/J	MGP_AJ_G0023286	protein coding gene	Chr17:23240950-23244189 (+)
AKR/J	MGP_AKRJ_G0023253	protein coding gene	Chr17:23329505-23332743 (+)
BALB/cJ	MGP_BALBcJ_G0023291	protein coding gene	Chr17:23441471-23444709 (+)
C3H/HeJ	MGP_C3HHeJ_G0023051	protein coding gene	Chr17:23694103-23697341 (+)
C57BL/6NJ	MGP_C57BL6NJ_G0023734	protein coding gene	Chr17:24967080-24970318 (+)
CAROLI/EiJ	MGP_CAROLIEiJ_G0021209	protein coding gene	Chr17:20701329-20704503 (+)
CAST/EiJ	MGP_CASTEiJ_G0022553	protein coding gene	Chr17:23549334-23552573 (+)
CBA/J	MGP_CBAJ_G0023027	protein coding gene	Chr17:25808393-25811631 (+)
DBA/2J	MGP_DBA2J_G0023156	protein coding gene	Chr17:22833613-22836852 (+)
FVB/NJ	MGP_FVBNJ_G0023126	protein coding gene	Chr17:22554167-22557405 (+)
LP/J	MGP_LPJ_G0023233	protein coding gene	Chr17:24209480-24212718 (+)
NOD/ShiLtJ	MGP_NODShiLtJ_G0023145	protein coding gene	Chr17:25500815-25504054 (+)
NZO/HlLtJ	MGP_NZOHlLtJ_G0023772	protein coding gene	Chr17:23613954-23617193 (+)
PWK/PhJ	MGP_PWKPhJ_G0022302	protein coding gene	Chr17:21589030-21592268 (+)
SPRET/EiJ	MGP_SPRETEiJ_G0022120	protein coding gene	Chr17:21678262-21681500 (+)
WSB/EiJ	MGP_WSBEiJ_G0022616	protein coding gene	Chr17:23686600-23689839 (+)

more

Human Ortholog

IGFALS, insulin like growth factor binding protein acid labile subunit

Vertebrate Orthologs

3

Vertebrate Orthology Source

Alliance of Genome Resources

Human Ortholog

IGFALS, insulin like growth factor binding protein acid labile subunit
Synonyms

ACLSD, ALS
Links

HGNC:5468

NCBI Gene ID: 3483

neXtProt AC: NX_P35858

UniProt: P35858
Chr Location

16p13.3; chr16:1790413-1794971 (-) GRCh38

MGI Vertebrate Homology

Igfals stringent orthology
1 human;1 mouse;1 rat;1 zebrafish
HCOP

vertebrate homology predictions: IGFALS
Gene Tree

Igfals

less

Phenotype Summary

7 phenotypes from 2 alleles in 3 genetic backgrounds
8 phenotypes from multigenic genotypes
1 images
17 phenotype references

Phenotype Overview

Phenotype Overview

Blue squares indicate phenotypes directly attributed to mutations/alleles of this gene.

adipose tissue	behavior/neurological	cardiovascular system	cellular	craniofacial	digestive/alimentary system	embryo	endocrine/exocrine glands	growth/size/body	hearing/vestibular/ear	hematopoietic system	homeostasis/metabolism	integument	immune system	limbs/digits/tail	liver/biliary system	mortality/aging	muscle	nervous system	pigmentation	renal/urinary system	reproductive system	respiratory system	skeleton	taste/olfaction	neoplasm	vision/eye

Click cells to view annotations.

All Mutations and Alleles

6
Endonuclease-mediated

2
Targeted

4
Incidental Mutations

Mutagenetix , APF
Find Mice (IMSR)

33 strains or lines available
Comparison Matrix

Gene Expression + Phenotype

Mice homozygous for disruptions in this gene gain weight more slowly after birth and display less growth in long bones.

less

All GO Annotations

10
GO References

6

Molecular Function

carbohydrate derivative binding	cytoskeletal protein binding	DNA binding	enzyme regulator	hydrolase	ligase	lipid binding	oxidoreductase	RNA binding	signaling receptor activity	signaling receptor binding	transcription	transferase	transporter

Biological Process

carbohydrate derivative metabolism	cell differentiation	cell population proliferation	cellular component organization	DNA-templated transcription	establishment of localization	homeostatic process	immune system process	lipid metabolic process	programmed cell death	protein metabolic process	response to stimulus	signaling	system development

Cellular Component

cell projection	cytoplasmic vesicle	cytoskeleton	cytosol	endoplasmic reticulum	endosome	extracellular region	Golgi apparatus	mitochondrion	non-membrane-bounded organelle	nucleus	organelle envelope	organelle lumen	plasma membrane	protein-containing complex	synapse	vacuole

Click cells to view annotations.

less

Expression Overview

Expression Overview

GXD's primary emphasis is on endogenous gene expression during development. Click on grid cells to view annotations.

Blue cells = expressed in wild-type.
Gray triangles = other expression annotations only
(e.g. absence of expression or data from mutants).

early conceptus	embryo ectoderm	embryo endoderm	embryo mesoderm	embryo mesenchyme	extraembryonic component	alimentary system	auditory system	branchial arches	cardiovascular system	connective tissue	endocrine system	exocrine system	hemolymphoid system	integumental system	limbs	liver and biliary system	musculoskeletal system	nervous system	olfactory system	reproductive system	respiratory system	urinary system	visual system

Click cells to view annotations.

Assay Results

711
Tissues

4
cDNA Data

46
Literature Summary

3

Tissue x Stage Matrix

Comparison Matrix

Gene Expression + Phenotype

Other Mouse Links

Allen Institute

GEO

Expression Atlas
Other Vertebrate Links

Xenbase igfals

ZFIN igfals

less

All Sequences

48
RefSeq

6
UniProt

5
CCDS

CCDS37497.1

Ensembl

ENSMUSG00000046070 (Evidence)
NCBI Gene

16005

Representative Sequences				Length	Strain/Species	Flank
	genomic	16005	NCBI Gene Model \| MGI Sequence Detail	4168	C57BL/6J	± kb
	transcript	NM_001364896	RefSeq \| MGI Sequence Detail	2232	ZRU/MplStud
	polypeptide	P70389	UniProt \| EBI \| MGI Sequence Detail	603	Not Applicable

less

UniProt

5 Sequences
Protein Ontology

PR:000008946 insulin-like growth factor-binding protein complex acid labile chain

(term hierarchy)
InterPro Domains

IPR000483 Cysteine-rich flanking region, C-terminal

IPR001611 Leucine-rich repeat

IPR032675 Leucine-rich repeat domain superfamily

IPR000372 Leucine-rich repeat N-terminal domain

IPR003591 Leucine-rich repeat, typical subtype

IPR050328 Multifunctional Developmental and Immune Receptor

IPR050333 Small Leucine-Rich Proteoglycans
GlyGen

P70389 7 sites

less

All nucleic 50

Genomic 3

cDNA 46

Primer pair 1

Microarray probesets 4

less

MGD-MRK-36553

more

Summaries

All 52

Developmental Gene Expression 3

Gene Ontology 6

Phenotypes 17
Earliest

J:35394 Boisclair YR, et al., Organization and chromosomal localization of the gene encoding the mouse acid labile subunit of the insulin-like growth factor binding complex. Proc Natl Acad Sci U S A. 1996 Sep 17;93(19):10028-33
Latest

J:345621 Adams DJ, et al., Genetic determinants of micronucleus formation in vivo. Nature. 2024 Mar;627(8002):130-136

TSS for Igfals:

(View these features in JBrowse)

Transcription Start Site	Location	Distance from Gene 5'-end
Tssr143101	Chr17:25096808-25096849 (+)	11 bp
Tssr143102	Chr17:25097199-25097238 (+)	401 bp
Tssr143103	Chr17:25097668-25097679 (+)	856 bp
Tssr143104	Chr17:25097698-25097755 (+)	909 bp
Tssr143105	Chr17:25097765-25097773 (+)	951 bp

Igfals is Candidate Gene for:

QTL	Genetic Location*	Genome Location (GRCm39)	Reference	QTL Note
Hdl4	Chr17, syntenic		J:99477	Authors used novel data mining tool ExQuest to identify novel candidate genes for existing diabesity QTLs. Next, candidate gene expression in the liver, adipose, and pancreas of diabesity-prone Tally Ho mice and diabesity-resistant C57BL/6J mice was assessed by quantitative PCR analysis. Several potential candidate genes, some with no previous association to diabesity QTLs, were identified. Since QTL intervals may be large and could contain hundreds or thousands of potential candidate genes, this method allows researchers to focus on those with strong potential as well as identify novel candidate genes. Potential candidate genes for Hdl4 (32.3 cM) on mouse Chromosome 17 as identified by ExQuest are Gnmt, Lrg1, and Sepx1 (10 cM). For QTL Insq5 (56.7 cM), potential candidate gene Abcg5 (54.5 cM) was identified. For QTL Obq4 (4 cM) and Wta4 (17 cM), potential candidate genes Plg (7.3 cM), Acat2 (7.55 cM), Acat3 (7.55 cM), Hagh (11 cM), Igfals, Decr2, Clps (17.1 cM), Tff1 (17 cM), Tff2 (17 cM), Tff3 (17 cM), and Apom were identified. Tff3 exhibits almost undetectable levels of transcription in the liver of Tally Ho animals compared C57BL/6J.
Insq5	Chr17, syntenic		J:99477	Authors used novel data mining tool ExQuest to identify novel candidate genes for existing diabesity QTLs. Next, candidate gene expression in the liver, adipose, and pancreas of diabesity-prone Tally Ho mice and diabesity-resistant C57BL/6J mice was assessed by quantitative PCR analysis. Several potential candidate genes, some with no previous association to diabesity QTLs, were identified. Since QTL intervals may be large and could contain hundreds or thousands of potential candidate genes, this method allows researchers to focus on those with strong potential as well as identify novel candidate genes. Potential candidate genes for Hdl4 (32.3 cM) on mouse Chromosome 17 as identified by ExQuest are Gnmt, Lrg1, and Sepx1 (10 cM). For QTL Insq5 (56.7 cM), potential candidate gene Abcg5 (54.5 cM) was identified. For QTL Obq4 (4 cM) and Wta4 (17 cM), potential candidate genes Plg (7.3 cM), Acat2 (7.55 cM), Acat3 (7.55 cM), Hagh (11 cM), Igfals, Decr2, Clps (17.1 cM), Tff1 (17 cM), Tff2 (17 cM), Tff3 (17 cM), and Apom were identified. Tff3 exhibits almost undetectable levels of transcription in the liver of Tally Ho animals compared C57BL/6J.
Obq4	Chr17, 4.92 cM		J:99477	Authors used novel data mining tool ExQuest to identify novel candidate genes for existing diabesity QTLs. Next, candidate gene expression in the liver, adipose, and pancreas of diabesity-prone Tally Ho mice and diabesity-resistant C57BL/6J mice was assessed by quantitative PCR analysis. Several potential candidate genes, some with no previous association to diabesity QTLs, were identified. Since QTL intervals may be large and could contain hundreds or thousands of potential candidate genes, this method allows researchers to focus on those with strong potential as well as identify novel candidate genes. Potential candidate genes for Hdl4 (32.3 cM) on mouse Chromosome 17 as identified by ExQuest are Gnmt, Lrg1, and Sepx1 (10 cM). For QTL Insq5 (56.7 cM), potential candidate gene Abcg5 (54.5 cM) was identified. For QTL Obq4 (4 cM) and Wta4 (17 cM), potential candidate genes Plg (7.3 cM), Acat2 (7.55 cM), Acat3 (7.55 cM), Hagh (11 cM), Igfals, Decr2, Clps (17.1 cM), Tff1 (17 cM), Tff2 (17 cM), Tff3 (17 cM), and Apom were identified. Tff3 exhibits almost undetectable levels of transcription in the liver of Tally Ho animals compared C57BL/6J.
Wta4	Chr17, 17.98 cM	Chr17:33819721-33819843	J:99477	Authors used novel data mining tool ExQuest to identify novel candidate genes for existing diabesity QTLs. Next, candidate gene expression in the liver, adipose, and pancreas of diabesity-prone Tally Ho mice and diabesity-resistant C57BL/6J mice was assessed by quantitative PCR analysis. Several potential candidate genes, some with no previous association to diabesity QTLs, were identified. Since QTL intervals may be large and could contain hundreds or thousands of potential candidate genes, this method allows researchers to focus on those with strong potential as well as identify novel candidate genes. Potential candidate genes for Hdl4 (32.3 cM) on mouse Chromosome 17 as identified by ExQuest are Gnmt, Lrg1, and Sepx1 (10 cM). For QTL Insq5 (56.7 cM), potential candidate gene Abcg5 (54.5 cM) was identified. For QTL Obq4 (4 cM) and Wta4 (17 cM), potential candidate genes Plg (7.3 cM), Acat2 (7.55 cM), Acat3 (7.55 cM), Hagh (11 cM), Igfals, Decr2, Clps (17.1 cM), Tff1 (17 cM), Tff2 (17 cM), Tff3 (17 cM), and Apom were identified. Tff3 exhibits almost undetectable levels of transcription in the liver of Tally Ho animals compared C57BL/6J.

*cM position of peak correlated region/marker

Contributing Projects: Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO)
Citing These Resources Funding Information Warranty Disclaimer, Privacy Notice, Licensing, & Copyright Send questions and comments to User Support.	last database update 10/29/2024 MGI 6.24