Publications by authors named "S M Gollin"

Prader-Willi syndrome (PWS) is a multisystem disorder with neurobehavioral, metabolic, and hormonal phenotypes, caused by loss of expression of a paternally-expressed imprinted gene cluster. Prior evidence from a PWS mouse model identified abnormal pancreatic islet development with retention of aged insulin and deficient insulin secretion. To determine the collective roles of PWS genes in β-cell biology, we used genome-editing to generate isogenic, clonal INS-1 insulinoma lines having 3.

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Phenylalanine hydroxylase-deficient (PAH-deficient) phenylketonuria (PKU) results in systemic hyperphenylalaninemia, leading to neurotoxicity with severe developmental disabilities. Dietary phenylalanine (Phe) restriction prevents the most deleterious effects of hyperphenylalaninemia, but adherence to diet is poor in adult and adolescent patients, resulting in characteristic neurobehavioral phenotypes. Thus, an urgent need exists for new treatments.

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The Consortium for Mouse Cell Line Authentication was formed to validate Short Tandem Repeat (STR) markers for intraspecies identification of mouse cell lines. The STR profiling method is a multiplex polymerase chain reaction (PCR) assay comprised of primers targeting 19 mouse STR markers and two human STR markers (for interspecies contamination screening). The goals of the Consortium were to perform an interlaboratory study to-(1) validate the mouse STR markers to uniquely identify mouse cell lines (intraspecies identification), (2) to provide a public database of mouse cell lines with the National Institute of Standards and Technology (NIST)-validated mouse STR profiles, and (3) to publish the results of the interlaboratory study.

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  • Cell lines are crucial for biological research and can help link genomic changes in tumors to new discoveries in treatment.
  • The study analyzed genomic and transcriptomic data from 15 HPV-negative and 11 HPV-positive head and neck cancer cell lines and compared them to 279 tumors from The Cancer Genome Atlas (TCGA).
  • Key findings include discovering gene amplifications in certain chromosome regions that lead to increased gene expression, revealing significant genetic patterns that could inform treatment strategies and highlight the worst prognoses for specific tumor types.
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  • Immunomodulatory drugs like lenalidomide and pomalidomide show significant effectiveness in treating multiple myeloma, but they often cause low platelet counts and increase the risk of developing other blood cancers.
  • These drugs promote the self-renewal of blood cell progenitors and boost the growth of megakaryocytic colonies by preventing cell death and encouraging the division of early megakaryocyte progenitors, primarily through the down-regulation of the IKZF1 gene.
  • The reduction of IKZF1 leads to decreased GATA1 levels, which affects various genes involved in megakaryocyte development, resulting in immature megakaryocytes and an overall increase in megakaryocytic progenitors, contributing to the
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