Kellie Parks scite author profile

Kellie Parks

3Publications

15Citation Statements Received

11Citation Statements Given

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George Washington University, Georgetown University Medical Center

Publications

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Discordance Between Cobas BRAF V600 Testing and VE1 Immunohistochemistry in a Melanoma Patient With Bone Marrow Metastases

Rapisuwon

Busam

Parks

et al. 2016

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False negative result remains an ongoing problem in direct gene sequencing of cancers. It is important to utilize the appropriate mutation detection method most appropriate to each circumstance and the available tissue. Here, we report a patient with melanoma of unknown primary with metastases to spleen and bone marrow, who was tested negative for Cobas BRAF V600E mutation, whose cancer progressed on anti-programmed death 1 (PD1) receptor monoclonal antibody therapy. Subsequent VE1 immunohistochemistry was positive for BRAF V600E mutation, and the tumor responded dramatically to BRAF/MEK inhibitor combination therapy. This demonstrates how alternative BRAF testing methodology could produce results that can influence treatment choice and the outcome.

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Novel somatic KIT exon 8 mutation with dramatic response to imatinib in a patient with mucosal melanoma

Rapisuwon

Parks²,

Al‐Refaie³

et al. 2014

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Primary mucosal melanomas represent ∼1.3% of all cases of melanoma diagnosed in the USA. The sinonasal location is the most common primary site. Mutations in the KIT gene occur in 10-22% of mucosal melanomas. Tumor response to imatinib mesylate has been reported in about half of the patients with tumors harboring KIT mutations. Responses are almost exclusively restricted to tumors with mutations in KIT exon 9 or 11. We report a case of a patient with a sinonasal mucosal melanoma with a novel exon 8 mutation (C443S) who had marked initial response to imatinib. Somatic exon 8 KIT mutations have not been previously reported in mucosal melanoma or in other human solid tumors; however, such mutations have been reported in canine and feline mast cell tumors. Protein transcripts from exon 8 play an important role in the structural and functional integrity of the extracellular domain of KIT. In preclinical studies, a mutation in exon 8 led to autophosphorylation, independent of KIT ligand, and constitutive activation of the tyrosine kinase. This biology may explain the successful application of imatinib in animals with tumors harboring exon 8 KIT mutations and in our patient with mucosal melanoma. This report expands the population of patients with melanoma who might benefit from imatinib to those with somatic exon 8 KIT mutations. Such mutations should be looked for in patients with mucosal melanoma.

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Novel somatic KIT exon 8 mutation and response to imatinib in a patient with mucosal melanoma: A case report.

Rapisuwon

Parks

Al‐Refaie

et al. 2014

JCO

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Kellie Parks

Discordance Between Cobas BRAF V600 Testing and VE1 Immunohistochemistry in a Melanoma Patient With Bone Marrow Metastases

Novel somatic KIT exon 8 mutation with dramatic response to imatinib in a patient with mucosal melanoma

Novel somatic KIT exon 8 mutation and response to imatinib in a patient with mucosal melanoma: A case report.

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