Full data view for gene PLN

The variants shown are described using the NM_002667.3 transcript reference sequence.

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Please note that a short description of a certain column can be displayed when you move your mouse cursor over the column's header and hold it still. Below, a more detailed description is shown per column.

Effect: The variant's effect on the function of the gene/protein, displayed in the format 'R/C'. R is the value reported by the source (publication, submitter) and this classification may vary between records. C is the value concluded by the curator. Note that in some database the curator uses Summary records to give details on the classification of the variant.Values used: '+' indicating the variant affects function, '+?' probably affects function, '-' does not affect function, '-?' probably does not affect function, '?' effect unknown, '.' effect was not classified.

Exon: Number of exon/intron containing variant; 2 = exon 2, 12i = intron 12, 2i_7i = exons 3 to 7, 8i_9 = border intron 8/exon 9.

DNA change (cDNA): Description of variant at DNA level, based on a coding DNA reference sequence (following HGVS recommendations); e.g. c.123C>T, c.123_145del, c.123_126dup.

RNA change: Description of variant at RNA level (following HGVS recommendations).

r.123c>u
r.? = unknown
r.(?) = RNA not analysed but probably transcribed copy of DNA variant
r.spl? = RNA not analysed but variant probably affects splicing
r.(spl?) = RNA not analysed but variant may affect splicing
r.0? = change expected to abolish transcription

Protein: Description of variant at protein level (following HGVS recommendations).

p.(Arg345Pro) = change predicted from DNA (RNA not analysed)
p.Arg345Pro = change derived from RNA analysis
p.? = unknown effect
p.0? = probably no protein produced

Allele: On which allele is the variant located? Does not necessarily imply inheritance! 'Paternal' (confirmed or inferred), 'Maternal' (confirmed or inferred), 'Parent #1' or #2 for compound heterozygosity without having screened the parents, 'Unknown' for heterozygosity without having screened the parents, 'Both' for homozygozity.

Type: Type of variant at DNA level; note that the variant type can also be derived from the variant description (for all levels).
All options:

Substitution
Deletion
Duplication
Insertion
Inversion
Insertion/Deletion
Translocation
Other/Complex

DNA change (genomic) (hg19): Description of variant at DNA level, based on the genomic DNA reference sequence (following HGVS recommendations).

g.12345678C>T
g.12345678_12345890del
g.12345678_12345890dup

Reference: Reference to publication describing the variant, including links to OMIM (when available), PubMed or or other source, e.g. "den Dunnen ASHG2003 P2346".

DB-ID: Database ID of variant, grouping multiple observations of the same variant together, starting with the HGNC gene symbol, followed by an underscore (_) and a six digit number (e.g. DMD_012345). _000000 is used for variants where DNA was not analysed (change predicted from RNA analysis), variants seen in animal models or variants not seen in humans but functionally tested in vitro.

Frequency: Frequency in which the variant was found; e.g 5/760 chromosomes (in 5 of 760 chromosomes tested), 1/33 patients (in 1 of 33 patients analysed in study), 0.05 controls (in 5% of control cases tested).

Variant remarks: Remarks regarding the variant described, e.g. germline mosaicism in mother, 345 kb deletion, muscle RNA analysed, not in 200 control chromosomes tested, on founder haplotype, etc.

ClassClinical: ClassClinical

Template: Template(s) used to detect the sequence variant; DNA = genomic DNA, RNA = RNA (cDNA).
All options:

DNA
RNA = RNA (cDNA)
Protein
? = unknown

Technique: Technique(s) used to identify the sequence variant.
All options:

? = Unknown
arrayCGH = array for Comparative Genomic Hybridisation
arraySEQ = array for resequencing
arraySNP = array for SNP typing
arrayCNV = array for Copy Number Variation (SNP and CNV probes)
BESS = Base Excision Sequence Scanning
CMC = Chemical Mismatch Cleavage
CSCE = Conformation Sensitive Capillary Electrophoresis
DGGE = Denaturing-Gradient Gel-Electrophoresis
DHPLC = Denaturing High-Performance Liquid Chromatography
DOVAM = Detection Of Virtually All Mutations (SSCA variant)
ddF = dideoxy Fingerprinting
DSCA = Double-Strand DNA Conformation Analysis
EMC = Enzymatic Mismatch Cleavage
HD = HeteroDuplex analysis
MCA = high-resolution Melting Curve Analysis (hrMCA)
IHC = Immuno-Histo-Chemistry
MAPH = Multiplex Amplifiable Probe Hybridisation
MLPA = Multiplex Ligation-dependent Probe Amplification
SEQ-NG = Next-Generation Sequencing
SEQ-NG-H = Next-Generation Sequencing - Helicos
SEQ-NG-I = Next-Generation Sequencing - Illumina/Solexa
SEQ-NG-R = Next-Generation Sequencing - Roche/454
SEQ-NG-S = Next-Generation Sequencing - SOLiD
Northern = Northern blotting
PCR = Polymerase Chain Reaction
PCRdig = PCR + restriction enzyme digestion
PCRlr = PCR, long-range
PCRm = PCR, multiplex
PCRq = PCR, quantitative
PAGE = Poly-Acrylamide Gel-Electrophoresis
PTT = Protein Truncation Test
PFGE = Pulsed-Field Gel-Electrophoresis (+Southern)
RT-PCR = Reverse Transcription and PCR
SEQ = SEQuencing
SBE = Single Base Extension
SSCA = Single-Strand DNA Conformation polymorphism Analysis (SSCP)
SSCAf = SSCA, fluorescent (SSCP)
Southern = Southern blotting
TaqMan = TaqMan assay
Western = Western Blotting

Reference: Reference to publication describing the individual/family, possibly giving more phenotypic details than listed in this database entry, including link to PubMed or other source, e.g. "den Dunnen ASHG2003 P2346". References in the "Country:City" format indicate that the variant was submitted directly to this database by the laboratory indicated.

Remarks: Remarks about the individual.

Gender: Gender

Age: Age

α-thal genotype: α-thal genotype

β-thal genotype: β-thal genotype

How to query this table

All list views have search fields which can be used to search data. You can search for a complete word or you can search for a part of a search term. If you enclose two or more words in double quotes, LOVD will search for the combination of those words only exactly in the order you specify. Note that search terms are case-insensitive and that wildcards such as * are treated as normal text! For all options, like "and", "or", and "not" searches, or searching for prefixes or suffixes, see the table below.

Operator	Column type	Example	Matches
	Text	Arg	all entries containing 'Arg'
space	Text	Arg Ser	all entries containing 'Arg' and 'Ser'
\|	Text	Arg\|Ser	all entries containing 'Arg' or 'Ser'
!	Text	!fs	all entries not containing 'fs'
^	Text	^p.(Arg	all entries beginning with 'p.(Arg'
$	Text	Ser)$	all entries ending with 'Ser)'
=""	Text	=""	all entries with this field empty
=""	Text	="p.0"	all entries exactly matching 'p.0'
!=""	Text	!=""	all entries with this field not empty
!=""	Text	!="p.0"	all entries not exactly matching 'p.0?'
combination	Text	*\|Ter !fs	all entries containing '*' or 'Ter' but not containing 'fs'
	Date	2020	all entries matching the year 2020
\|	Date	2020-03\|2020-04	all entries matching March or April, 2020
!	Date	!2020-03	all entries not matching March, 2020
<	Date	<2020	all entries before the year 2020
<=	Date	<=2020-06	all entries in or before June, 2020
>	Date	>2020-06	all entries after June, 2020
>=	Date	>=2020-06-15	all entries on or after June 15th, 2020
combination	Date	2019\|2020 <2020-03	all entries in 2019 or 2020, and before March, 2020
	Numeric	23	all entries exactly matching 23
\|	Numeric	23\|24	all entries exactly matching 23 or 24
!	Numeric	!23	all entries not exactly matching 23
<	Numeric	<23	all entries lower than 23
<=	Numeric	<=23	all entries lower than, or equal to, 23
>	Numeric	>23	all entries higher than 23
>=	Numeric	>=23	all entries higher than, or equal to, 23
combination	Numeric	>=20 <30 !23	all entries with values from 20 to 29, but not equal to 23

Some more advanced examples:

Example	Matches
Asian	all entries containing 'Asian', 'asian', including 'Caucasian', 'caucasian', etc.
Asian !Caucasian	all entries containing 'Asian' but not containing 'Caucasian'
Asian\|African !Caucasian	all entries containing 'Asian' or 'African', but not containing 'Caucasian'
"South Asian"	all entries containing 'South Asian', but not containing 'South East Asian'

To sort on a certain column, click on the column header or on the arrows. If that column is already selected to sort on, the sort order will be swapped. The column currently sorted on has a darker blue background color than the other columns. The up and down arrows next to the column name indicate the current sorting direction. When sorting on any field other than the default, LOVD will sort secondarily on the default sort column.

17 entries on 1 page. Showing entries 1 - 17.

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How to query

Effect	Exon	DNA change (cDNA)	RNA change	Protein	Allele	Type	DNA change (genomic) (hg19)	Reference	DB-ID	Frequency	Variant remarks	ClassClinical	Template	Technique	Disease	Reference	Remarks	Gender	Age	α-thal genotype	β-thal genotype	Panel size	Owner
./.	02	c.-42C>G	-	-	Unknown	Substitution	-	GenBank	PLN_00008	-	Otherwise, mutations in the PLN gene are not a frequent cause of cardiomyopathies in our population.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.	-	-	Unknown	Substitution	-	GenBank	PLN_00006	-	we identified a novel variant (	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.?	-	-	Unknown	Substitution	-	GenBank	PLN_00001	-	The mutation site is within the region that plays a critical role in expression of the PLN gene [11,13] and is close to a very conserved CCAAT element ()84 to )80), on which the nuclear protein NF-Y binds to reg- ulate the PLN promoter activity.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.25C>T	-	p.Arg9Cys	Unknown	Substitution	-	GenBank	PLN_00002	-	These results indicate that myocellular calcium dysregulation can initiate human heart failure	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.25C>T	-	p.Arg9Cys	Unknown	Substitution	-	GenBank	PLN_00002	-	This result idicated that PLN gene mutation may not be a common cause for DCM in the Chinese population in Chengdu.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.25C>T	-	p.Arg9Cys	Unknown	Substitution	-	GenBank	PLN_00002	-	Based on coimmunoprecipitation experiments proposed that PLNR9C binds PKA-C irreversibly, creating dead- end complexes that deplete the local reservoir of kinase.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.25C>T	-	p.Arg9Cys	Unknown	Substitution	-	GenBank	PLN_00002	-	The sequence analysis of selected coding regions of the PLN gene did not show the presence of mutations in either the patient or the control subpopulations.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.39_42delAAGAinsG	-	p.Arg14del	Unknown	Insertion/Deletion	-	GenBank	PLN_00011	-	chronic suppression of either basal SERCA2a activity (PLN-R14Del mutant) or the stimulatory effect of the -adrenergic signaling pathway (PLN-R9C mutant) (11) result in human cardiomyopathy and heart failure;absence of PLN inhibition by the PLN-L39stop mutant, associated with the lack of regulatory inhibition of SERCA2a and increased cardiac work, may also result in heart failure.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.39_42delAAGAinsG	-	p.Arg14del	Unknown	Insertion/Deletion	-	GenBank	PLN_00011	-	It cannot be determined whether R13 or R14 is deleted because the codon for each is identical. The deletion of either R13 or R14 is expected to partially disrupt the stability of the pentamer structure of this 52 amino acid protein.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.41G>T	-	p.Arg14Ile	Unknown	Substitution	-	GenBank	PLN_00012	-	-	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.46T>G	-	p.Ser16Ala	Unknown	Substitution	-	GenBank	PLN_00004	-	that phosphorylation of Thr in PLN plays an important role in positive frequency and contraction relationship in mouse cardiomyocytes.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.49A>G	-	p.Thr17Ala	Unknown	Substitution	-	GenBank	PLN_00005	-	Phosphorylation of Thr 17 in PLN plays an important role in positive frequency and contraction relationship in mouse cardiomyocytes.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.116T>G	-	p.Leu39X	Unknown	Substitution	-	GenBank	PLN_00003	-	These findings describe a naturallyoccurring loss-of-function human PLN mutation (PLN null). In contrast to reported benefits of PLN ablation in mouse heart failure, humans lacking PLN develop lethal dilated cardiomyopathy.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.116T>G	-	p.Leu39X	Unknown	Substitution	-	GenBank	PLN_00003	-	This result indicated that PLN gene mutation may not be a common cause for DCM in the Chinese population in Chengdu.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.116T>G	-	p.Leu39X	Unknown	Substitution	-	GenBank	PLN_00003	-	Mutations in PLN, such as the L39X, are rare among patients with HCM. However, despite the low yield of PLN-associated HCM genetic testing, the small size of PLN and the paucity of genetic variation in PLN among healthy subjects warrant consideration for its inclusion in clinically available HCM gene test panels.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.116T>G	-	p.Leu39X	Unknown	Substitution	-	GenBank	PLN_00003	-	The sequence analysis of selected coding regions of the PLN gene did not show the presence of mutations in either the patient or the control subpopulations.	-	-	-	-	-	-	-	-	-	-	-	-
./.	02	c.116T>G	-	p.Leu39X	Unknown	Substitution	-	GenBank	PLN_00003	-	The heterozygous carriers of the Leu39Ter mutation exhibited asymptomatic hypertrophic cardiomyopathy without diminished contractile performance. Homozygous carriers of this mutation developed a severe form of DCM resulting in heart failure requiring cardiac transplantation at a young age [10]. Additional studies have identified other mutations in PLN causing DCM [5,11,12] and mutations in the promoter region that may result in FHC [13,14]. Mutations in the PLN gene are likely to lead to a cardiomyopathic phenotype.	-	-	-	-	-	-	-	-	-	-	-	-

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Zhejiang University Center for Genetic and Genomic Medicine (ZJU-CGGM)

PLN (phospholamban)