Entry - *604174 - RIBOSOMAL PROTEIN L15; RPL15 - OMIM

 
 
* 604174

RIBOSOMAL PROTEIN L15; RPL15


HGNC Approved Gene Symbol: RPL15

Cytogenetic location: 3p24.2   Genomic coordinates (GRCh38) : 3:23,916,545-23,924,631 (from NCBI)


Gene-Phenotype Relationships
Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key
3p24.2 Diamond-Blackfan anemia 12 615550 AD 3

TEXT

Description

The mammalian ribosome is composed of 4 RNA species (see 180450) and approximately 80 different proteins (see 180466).

Cloning and Expression

Adams et al. (1992) isolated an RPL15 cDNA as a human brain EST that shows sequence similarity to the yeast ribosomal protein YL10 gene.

The complete coding sequence of the human RPL15 gene has been deposited in GenBank (L25899). The deduced RPL15 protein has 205 amino acids.

Gene Function

In mice, Ebright et al. (2020) conducted an in vivo genomewide CRISPR activation screen in circulating tumor cells from breast cancer patients to identify genes that promote distant metastasis. Genes coding for ribosomal proteins and regulators of translation were enriched in this screen. Overexpression of RPL15 increased metastatic growth in multiple organs and selectively enhanced translation of other ribosomal proteins and cell cycle regulators. RNA sequencing of freshly isolated circulating tumor cells from breast cancer patients revealed a subset with strong ribosome and protein synthesis signatures; these circulating tumor cells expressed proliferation and epithelial markers and correlated with poor clinical outcome.


Mapping

By somatic cell hybrid and radiation hybrid mapping analyses, Kenmochi et al. (1998) mapped the human RPL15 gene to 3p.

Gross (2013) mapped the RPL15 gene to chromosome 3p24.2 based on an alignment of the RPL15 sequence (GenBank AF279903) with the genomic sequence (GRCh37).

Molecular Genetics

Landowski et al. (2013) performed array CGH for copy number variation in 87 probands with Diamond-Blackfan anemia (DBA12; 615550) who were negative for mutation in 10 known DBA-associated ribosomal protein genes, and identified a large deletion in the RPL15 gene in 1 patient (604174.0001).

Wlodarski et al. (2018) identified heterozygous nonsense and missense mutations in the RPL15 gene in 6 unrelated patients with DBA12 (604174.0002-604174.0005). One of the nonsense mutations (Y81X; 604174.0002) was found in 3 patients. The mutations were identified by Sanger sequencing of the RPL15 gene in a cohort of 985 patients with DBA without a molecular diagnosis. Lymphoblastoid cells from 2 of the patients with the Y81X mutation showed impaired pre-rRNA processing, decreased 60S ribosomal subunit formation, and deficient cell proliferation. Bone marrow mononuclear cells from these 2 patients also showed increased TP53-induced apoptosis and increased p21 mRNA and delayed erythrocyte maturation compared to wildtype cells.


Genotype/Phenotype Correlations

Wlodarski et al. (2018) identified heterozygous nonsense mutations in the RPL15 gene in 4 unrelated patients with DBS12, 3 with a Y81X mutation (604174.0002) and 1 with a Q29X mutation (604174.0003). Three of these patients had hydrops fetalis, which is a rare presentation in DBA. The 3 patients with a Y81X mutation achieved rapid treatment independence, both with or without steroid therapy. This treatment independence was not due to gene mutation reversion.


ALLELIC VARIANTS ( 5 Selected Examples):

.0001 DIAMOND-BLACKFAN ANEMIA 12

RPL15, 2,393-BP DEL
   RCV000074478

In a female patient with Diamond-Blackfan anemia (DBA12; 615550), Landowski et al. (2013) identified heterozygosity for a 2,393-bp deletion at chr3:23,935,161-23,937,553 (NCBI36), containing all of exon 4 of the RPL15 gene (EX4DEL). Validation by mPCR showed that only the PCR product from exon 4 was significantly decreased; mPCR in unaffected family members showed ratios more similar to controls than to the proband. Functional analysis by knockdown of RPL15 in HeLa cells showed a drop in free 60S ribosomal subunits and the appearance of half-mers in the polysome profile, characteristic of defective 60S subunit production. There were also decreased levels of 32S and 12S pre-rRNAs, precursors to the 5.8S and 28S rRNAs. In addition, there was accumulation of the 41S, 30S, and 18S-E pre-rRNAs relative to the 21S pre-rRNA, suggesting a defect in internal transcribed spacer-1 (ITS1) cleavage at site 2. Analysis of RNA from patient lymphoblastoid cell lines showed a pattern consistent with the findings in the knocked-down HeLa cells, strongly suggesting that the RPL15 deletion affects pre-rRNA processing in patient cells.


.0002 DIAMOND-BLACKFAN ANEMIA 12

RPL15, TYR81TER
   RCV003228754...

In 3 unrelated patients (patients 1-3) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a 1-bp duplication (c.242dupA, NM_001253379.1) in the RPL15 gene, resulting in a tyr81-to-ter (Y81X) substitution. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The father of one of the patients (patient 1) also carried the mutation and was determined to be a silent carrier due to high erythrocyte adenosine deaminase levels. The mutation occurred de novo in the other 2 patients. The variant was not present in the ExAC and gnomAD databases. Lymphoblastoid cells from 2 of the patients showed impaired pre-rRNA processing, decreased 60S ribosomal subunit formation, and deficient cell proliferation.


.0003 DIAMOND-BLACKFAN ANEMIA 12

RPL15, GLN29TER
   RCV003228755

In a patient (patient 4) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.85C-T transition (c.85C-T, NM_001253379.1) in the RPL15 gene, resulting in a gln29-to-ter (Q29X) substitution. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The parents were not tested for the mutation. The variant was not present in the ExAC and gnomAD databases.


.0004 DIAMOND-BLACKFAN ANEMIA 12

RPL15, LEU10PRO
   RCV003228756

In a patient (patient 5) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.29T-C transition (c.29T-C, NM_001253379.1) in the RPL15 gene, resulting in a leu10-to-pro (L10P) substitution at a conserved site. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The mutation was inherited from the patient's mother. The variant was not present in the ExAC and gnomAD databases.


.0005 DIAMOND-BLACKFAN ANEMIA 12

RPL15, LYS153THR
   RCV003228757

In a patient (patient 6) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.458A-C transversion (c.458A-C, NM_001253379.1) in the RPL15 gene, resulting in a lys153-to-thr (K153T) substitution at a conserved site. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The parents were not tested for the mutation. The variant was present in 33 of 232,840 alleles in the gnomAD database.


REFERENCES

  1. Adams, M. D., Dubnick, M., Kerlavage, A. R., Moreno, R., Kelley, J. M., Utterback, T. R., Nagle, J. W., Fields, C., Venter, J. C. Sequence identification of 2,375 human brain genes. Nature 355: 632-634, 1992. Note: Comment: Nature 357: 367-368, 1992. [PubMed: 1538749, related citations] [Full Text]

  2. Ebright, R. Y., Lee, S., Wittner, B. S., Niederhoffer, K. L., Nicholson, B. T., Bardia, A., Truesdell, S., Wiley, D. F., Wesley, B., Li, S., Mai, A., Aceto, N., and 13 others. Deregulation of ribosomal protein expression and translation promotes breast cancer metastasis. Science 367: 1468-1473, 2020. [PubMed: 32029688, images, related citations] [Full Text]

  3. Gross, M. B. Personal Communication. Baltimore, Md. 12/19/2013.

  4. Kenmochi, N., Kawaguchi, T., Rozen, S., Davis, E., Goodman, N., Hudson, T. J., Tanaka, T., Page, D. C. A map of 75 human ribosomal protein genes. Genome Res. 8: 509-523, 1998. [PubMed: 9582194, related citations] [Full Text]

  5. Landowski, M., O'Donohue, M.-F., Buros, C., Ghazvinian, R., Montel-Lehry, N., Vlachos, A., Sieff, C. A., Newburger, P. E., Niewiadomska, E., Matysiak, M., Glader, B., Atsidaftos, E., Lipton, J. M., Beggs, A. H., Gleizes, P.-E., Gazda, H. T. Novel deletion of RPL15 identified by array-comparative genomic hybridization in Diamond-Blackfan anemia. Hum. Genet. 132: 1265-1274, 2013. [PubMed: 23812780, images, related citations] [Full Text]

  6. Wlodarski, M. W., Da Costa, L., O'Donohue, M. F., Gastou, M., Karboul, N., Montel-Lehry, N., Hainmann, I., Danda, D., Szvetnik, A., Pastor, V., Paolini, N., di Summa, F. M., Tamary, H., Quider, A. A., Aspesi, A., Houtkooper, R. H., Leblanc, T., Niemeyer, C. M., Gleizes, P. E., MacInnes, A. W. Recurring mutations in RPL15 are linked to hydrops fetalis and treatment independence in Diamond-Blackfan anemia. Haematologica 103: 949-958, 2018. [PubMed: 29599205, images, related citations] [Full Text]


Contributors:
Hilary J. Vernon - updated : 05/17/2023
Ada Hamosh - updated : 06/17/2020
Matthew B. Gross - updated : 12/19/2013
Marla J. F. O'Neill - updated : 11/27/2013
Creation Date:
Patti M. Sherman : 9/17/1999
Edit History:
carol : 05/18/2023
carol : 05/17/2023
carol : 06/18/2020
alopez : 06/17/2020
alopez : 02/06/2015
carol : 6/21/2014
mgross : 12/19/2013
carol : 12/2/2013
mcolton : 11/27/2013
psherman : 12/7/1999
mgross : 9/20/1999
psherman : 9/17/1999

* 604174

RIBOSOMAL PROTEIN L15; RPL15


HGNC Approved Gene Symbol: RPL15

Cytogenetic location: 3p24.2   Genomic coordinates (GRCh38) : 3:23,916,545-23,924,631 (from NCBI)


Gene-Phenotype Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key
3p24.2 Diamond-Blackfan anemia 12 615550 Autosomal dominant 3

TEXT

Description

The mammalian ribosome is composed of 4 RNA species (see 180450) and approximately 80 different proteins (see 180466).

Cloning and Expression

Adams et al. (1992) isolated an RPL15 cDNA as a human brain EST that shows sequence similarity to the yeast ribosomal protein YL10 gene.

The complete coding sequence of the human RPL15 gene has been deposited in GenBank (L25899). The deduced RPL15 protein has 205 amino acids.

Gene Function

In mice, Ebright et al. (2020) conducted an in vivo genomewide CRISPR activation screen in circulating tumor cells from breast cancer patients to identify genes that promote distant metastasis. Genes coding for ribosomal proteins and regulators of translation were enriched in this screen. Overexpression of RPL15 increased metastatic growth in multiple organs and selectively enhanced translation of other ribosomal proteins and cell cycle regulators. RNA sequencing of freshly isolated circulating tumor cells from breast cancer patients revealed a subset with strong ribosome and protein synthesis signatures; these circulating tumor cells expressed proliferation and epithelial markers and correlated with poor clinical outcome.


Mapping

By somatic cell hybrid and radiation hybrid mapping analyses, Kenmochi et al. (1998) mapped the human RPL15 gene to 3p.

Gross (2013) mapped the RPL15 gene to chromosome 3p24.2 based on an alignment of the RPL15 sequence (GenBank AF279903) with the genomic sequence (GRCh37).

Molecular Genetics

Landowski et al. (2013) performed array CGH for copy number variation in 87 probands with Diamond-Blackfan anemia (DBA12; 615550) who were negative for mutation in 10 known DBA-associated ribosomal protein genes, and identified a large deletion in the RPL15 gene in 1 patient (604174.0001).

Wlodarski et al. (2018) identified heterozygous nonsense and missense mutations in the RPL15 gene in 6 unrelated patients with DBA12 (604174.0002-604174.0005). One of the nonsense mutations (Y81X; 604174.0002) was found in 3 patients. The mutations were identified by Sanger sequencing of the RPL15 gene in a cohort of 985 patients with DBA without a molecular diagnosis. Lymphoblastoid cells from 2 of the patients with the Y81X mutation showed impaired pre-rRNA processing, decreased 60S ribosomal subunit formation, and deficient cell proliferation. Bone marrow mononuclear cells from these 2 patients also showed increased TP53-induced apoptosis and increased p21 mRNA and delayed erythrocyte maturation compared to wildtype cells.


Genotype/Phenotype Correlations

Wlodarski et al. (2018) identified heterozygous nonsense mutations in the RPL15 gene in 4 unrelated patients with DBS12, 3 with a Y81X mutation (604174.0002) and 1 with a Q29X mutation (604174.0003). Three of these patients had hydrops fetalis, which is a rare presentation in DBA. The 3 patients with a Y81X mutation achieved rapid treatment independence, both with or without steroid therapy. This treatment independence was not due to gene mutation reversion.


ALLELIC VARIANTS 5 Selected Examples):

.0001   DIAMOND-BLACKFAN ANEMIA 12

RPL15, 2,393-BP DEL
ClinVar: RCV000074478

In a female patient with Diamond-Blackfan anemia (DBA12; 615550), Landowski et al. (2013) identified heterozygosity for a 2,393-bp deletion at chr3:23,935,161-23,937,553 (NCBI36), containing all of exon 4 of the RPL15 gene (EX4DEL). Validation by mPCR showed that only the PCR product from exon 4 was significantly decreased; mPCR in unaffected family members showed ratios more similar to controls than to the proband. Functional analysis by knockdown of RPL15 in HeLa cells showed a drop in free 60S ribosomal subunits and the appearance of half-mers in the polysome profile, characteristic of defective 60S subunit production. There were also decreased levels of 32S and 12S pre-rRNAs, precursors to the 5.8S and 28S rRNAs. In addition, there was accumulation of the 41S, 30S, and 18S-E pre-rRNAs relative to the 21S pre-rRNA, suggesting a defect in internal transcribed spacer-1 (ITS1) cleavage at site 2. Analysis of RNA from patient lymphoblastoid cell lines showed a pattern consistent with the findings in the knocked-down HeLa cells, strongly suggesting that the RPL15 deletion affects pre-rRNA processing in patient cells.


.0002   DIAMOND-BLACKFAN ANEMIA 12

RPL15, TYR81TER
ClinVar: RCV003228754, RCV003973781, RCV004697276

In 3 unrelated patients (patients 1-3) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a 1-bp duplication (c.242dupA, NM_001253379.1) in the RPL15 gene, resulting in a tyr81-to-ter (Y81X) substitution. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The father of one of the patients (patient 1) also carried the mutation and was determined to be a silent carrier due to high erythrocyte adenosine deaminase levels. The mutation occurred de novo in the other 2 patients. The variant was not present in the ExAC and gnomAD databases. Lymphoblastoid cells from 2 of the patients showed impaired pre-rRNA processing, decreased 60S ribosomal subunit formation, and deficient cell proliferation.


.0003   DIAMOND-BLACKFAN ANEMIA 12

RPL15, GLN29TER
ClinVar: RCV003228755

In a patient (patient 4) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.85C-T transition (c.85C-T, NM_001253379.1) in the RPL15 gene, resulting in a gln29-to-ter (Q29X) substitution. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The parents were not tested for the mutation. The variant was not present in the ExAC and gnomAD databases.


.0004   DIAMOND-BLACKFAN ANEMIA 12

RPL15, LEU10PRO
ClinVar: RCV003228756

In a patient (patient 5) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.29T-C transition (c.29T-C, NM_001253379.1) in the RPL15 gene, resulting in a leu10-to-pro (L10P) substitution at a conserved site. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The mutation was inherited from the patient's mother. The variant was not present in the ExAC and gnomAD databases.


.0005   DIAMOND-BLACKFAN ANEMIA 12

RPL15, LYS153THR
ClinVar: RCV003228757

In a patient (patient 6) with Diamond-Blackfan anemia (DBA12; 615550), Wlodarski et al. (2018) identified heterozygosity for a c.458A-C transversion (c.458A-C, NM_001253379.1) in the RPL15 gene, resulting in a lys153-to-thr (K153T) substitution at a conserved site. The mutation was identified by Sanger sequencing of the RPL15 gene in a cohort of patients with DBA without a molecular diagnosis. The parents were not tested for the mutation. The variant was present in 33 of 232,840 alleles in the gnomAD database.


REFERENCES

  1. Adams, M. D., Dubnick, M., Kerlavage, A. R., Moreno, R., Kelley, J. M., Utterback, T. R., Nagle, J. W., Fields, C., Venter, J. C. Sequence identification of 2,375 human brain genes. Nature 355: 632-634, 1992. Note: Comment: Nature 357: 367-368, 1992. [PubMed: 1538749] [Full Text: https://doi.org/10.1038/355632a0]

  2. Ebright, R. Y., Lee, S., Wittner, B. S., Niederhoffer, K. L., Nicholson, B. T., Bardia, A., Truesdell, S., Wiley, D. F., Wesley, B., Li, S., Mai, A., Aceto, N., and 13 others. Deregulation of ribosomal protein expression and translation promotes breast cancer metastasis. Science 367: 1468-1473, 2020. [PubMed: 32029688] [Full Text: https://doi.org/10.1126/science.aay0939]

  3. Gross, M. B. Personal Communication. Baltimore, Md. 12/19/2013.

  4. Kenmochi, N., Kawaguchi, T., Rozen, S., Davis, E., Goodman, N., Hudson, T. J., Tanaka, T., Page, D. C. A map of 75 human ribosomal protein genes. Genome Res. 8: 509-523, 1998. [PubMed: 9582194] [Full Text: https://doi.org/10.1101/gr.8.5.509]

  5. Landowski, M., O'Donohue, M.-F., Buros, C., Ghazvinian, R., Montel-Lehry, N., Vlachos, A., Sieff, C. A., Newburger, P. E., Niewiadomska, E., Matysiak, M., Glader, B., Atsidaftos, E., Lipton, J. M., Beggs, A. H., Gleizes, P.-E., Gazda, H. T. Novel deletion of RPL15 identified by array-comparative genomic hybridization in Diamond-Blackfan anemia. Hum. Genet. 132: 1265-1274, 2013. [PubMed: 23812780] [Full Text: https://doi.org/10.1007/s00439-013-1326-z]

  6. Wlodarski, M. W., Da Costa, L., O'Donohue, M. F., Gastou, M., Karboul, N., Montel-Lehry, N., Hainmann, I., Danda, D., Szvetnik, A., Pastor, V., Paolini, N., di Summa, F. M., Tamary, H., Quider, A. A., Aspesi, A., Houtkooper, R. H., Leblanc, T., Niemeyer, C. M., Gleizes, P. E., MacInnes, A. W. Recurring mutations in RPL15 are linked to hydrops fetalis and treatment independence in Diamond-Blackfan anemia. Haematologica 103: 949-958, 2018. [PubMed: 29599205] [Full Text: https://doi.org/10.3324/haematol.2017.177980]


Contributors:
Hilary J. Vernon - updated : 05/17/2023
Ada Hamosh - updated : 06/17/2020
Matthew B. Gross - updated : 12/19/2013
Marla J. F. O'Neill - updated : 11/27/2013

Creation Date:
Patti M. Sherman : 9/17/1999

Edit History:
carol : 05/18/2023
carol : 05/17/2023
carol : 06/18/2020
alopez : 06/17/2020
alopez : 02/06/2015
carol : 6/21/2014
mgross : 12/19/2013
carol : 12/2/2013
mcolton : 11/27/2013
psherman : 12/7/1999
mgross : 9/20/1999
psherman : 9/17/1999



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.
Printed: March 5, 2025