Joshua Farhadian, FAAD, MD
Assistant Professor Adjunct - DermatologyCards
Contact Info
About
Titles
Assistant Professor Adjunct - Dermatology
Biography
Joshua Farhadian, MD, is a fellowship-trained Mohs micrographic surgeon with clinical expertise in the diagnosis, treatment, and prevention of skin cancers.
Dr. Farhadian graduated summa cum laude from the University of Pennsylvania and went on to attend medical school at New York University School of Medicine, where he graduated with Honors. While in medical school, he received the prestigious Marion B. Sulzberger Award for Excellence in Dermatology and conducted a year of laboratory research with the Interdisciplinary Melanoma Cooperative Group at New York University School of Medicine. After receiving his M.D., Dr. Farhadian completed his medical internship at Memorial Sloan Kettering Cancer Center and then returned to New York University for his dermatology residency. During this time, he was elected Chief Resident and received the Morris Leider Award for Best Graduating Resident. After residency, he pursued further specialty training at Yale School of Medicine, where he completed a fellowship in Mohs Micrographic Surgery and Dermatologic Oncology.
Departments & Organizations
- All Institutions
- Yale New Haven Health System
Education & Training
- Fellowship
- Yale School of Medicine (2018)
- Residency
- New York University School of Medicine (2017)
- Internship
- Memorial Sloan Kettering Cancer Center (2014)
- MD
- New York University School of Medicine
- BA
- University of Pennsylvania
Board Certifications
Dermatology
- Certification Organization
- AB of Dermatology
- Original Certification Date
- 2017
Research
Overview
My interest in cancer research stems from my childhood, when a close family was diagnosed with leukemia.
While an undergraduate at the University of Pennsylvania, I had my first cancer research experience working in a lab at the Feinstein Institute for Medical Research. My research there focused on the mechanism by which a protein named MRK is activated and mediates cell cycle arrest in response to ionizing radiation. Subsequently, while a medical student in the honors program at New York University School of Medicine, I continued performing cancer research in the Philips Lab, where I investigated the regulation of a molecule named isoprenylcysteine carboxymethyl transferase (ICMT), which is a protein that plays a role in approximately 25% of all cancers, including skin cancers.
As a medical student at NYU, I completed a year-long research fellowship with the Interdisciplinary Melanoma Cooperative Group (IMCG) at NYU. Supported by grants from the American Medical Association and the American Skin Association, I, along with my colleagues, uncovered nodular melanoma-specific molecular alterations that are pharmacologically targetable in vitro. Additionally, through our work on melanoma brain metastases and microRNA expression in BRAF mutant primary tumors, we identified previously unknown characteristics of melanoma that may one-day influence its management and treatment.
Since medical school, I have been involved a variety of skin cancer related clinical studies. Most recently, my colleagues and I have researched histologic phenotypes that impart aggressive behavior in squamous cell carcinoma. By identifying high risk features, we hope to help stratify patient
Research at a Glance
Yale Co-Authors
Publications Timeline
Jonathan Leventhal, MD
Publications
2018
Pulsed Dye Laser at Subpurpuric Settings for the Treatment of Pulsed Dye Laser–Induced Ecchymoses in Patients With Port-Wine Stains
Brauer JA, Farhadian JA, Bernstein LJ, Bae YS, Geronemus RG. Pulsed Dye Laser at Subpurpuric Settings for the Treatment of Pulsed Dye Laser–Induced Ecchymoses in Patients With Port-Wine Stains. Dermatologic Surgery 2018, 44: 220-226. PMID: 28858925, DOI: 10.1097/dss.0000000000001255.Peer-Reviewed Original ResearchCitationsMeSH Keywords and ConceptsConceptsPort-wine stainsTreatment of PWSSignificant adverse eventsPulsed dye laserAdverse eventsClinical improvementTreatment sideMajor complaintMasked evaluatorsEcchymosisFirst treatmentTreatment seriesControl sidePatientsSecond treatmentPWS clearancePurpuraTreatmentBruisingStainPDLSettingMean valueLesionsExtremities
2016
Trimethoprim-Sulfamethoxazole-Induced Subcutaneous Sweet's Syndrome Masquerading as Septic Shock
Hase J, Ma H, Wu B, Adelman M, Farhadian J, Femia A, Meehan S, Schwartz D. Trimethoprim-Sulfamethoxazole-Induced Subcutaneous Sweet's Syndrome Masquerading as Septic Shock. CHEST Journal 2016, 150: 376a. DOI: 10.1016/j.chest.2016.08.389.Peer-Reviewed Original ResearchCitationsPrimary cutaneous marginal-zone lymphoma.
Farhadian J, Terushkin V, Meehan SA, Latkowski JA. Primary cutaneous marginal-zone lymphoma. Dermatology Online Journal 2016, 22 PMID: 28329553, DOI: 10.5070/d32212033397.Peer-Reviewed Original ResearchCitationsMeSH Keywords and ConceptsSkin-limited relapse of systemic anaplastic large-cell lymphoma.
Farhadian JA, Terushkin V, Meehan SA, Kornreich C. Skin-limited relapse of systemic anaplastic large-cell lymphoma. Dermatology Online Journal 2016, 22 PMID: 28329531, DOI: 10.5070/d32212033374.Peer-Reviewed Original Research
2015
Male Aesthetics: A Review of Facial Anatomy and Pertinent Clinical Implications.
Farhadian JA, Bloom BS, Brauer JA. Male Aesthetics: A Review of Facial Anatomy and Pertinent Clinical Implications. Journal Of Drugs In Dermatology 2015, 14: 1029-34. PMID: 26355624.Peer-Reviewed Original ResearchCitationsAltmetricMeSH Keywords and ConceptsConceptsCosmetic proceduresBlood vessel densityAesthetic proceduresPertinent clinical implicationsInvasive cosmetic proceduresMale patientsNumber of menPatient dissatisfactionMuscle massVessel densitySubcutaneous tissueClinical implicationsImproper techniqueCosmetic dermatologyFacial anatomyMenDermatologyFacial proportionsAnatomyFemalesTreatment parametersPatientsRSK1 activation promotes invasion in nodular melanoma
Salhi A, Farhadian J, Giles K, de Miera E, Silva I, Bourque C, Yeh K, Chhangawala S, Wang J, Ye F, Zhang D, Hernando E, Houvras Y, Osman I. RSK1 activation promotes invasion in nodular melanoma. Journal Of Translational Medicine 2015, 13: o2. PMCID: PMC4315266, DOI: 10.1186/1479-5876-13-s1-o2.Peer-Reviewed Original ResearchRSK1 Activation Promotes Invasion in Nodular Melanoma
Salhi A, Farhadian JA, Giles KM, de Miera E, Silva IP, Bourque C, Yeh K, Chhangawala S, Wang J, Ye F, Zhang DY, Hernando-Monge E, Houvras Y, Osman I. RSK1 Activation Promotes Invasion in Nodular Melanoma. American Journal Of Pathology 2015, 185: 704-716. PMID: 25579842, PMCID: PMC4348467, DOI: 10.1016/j.ajpath.2014.11.021.Peer-Reviewed Original ResearchMeSH Keywords and ConceptsConceptsRibosomal protein S6 kinaseGene expression microarray analysisProtein S6 kinaseExpression microarray analysisMelanoma cellsSer-380RSK1 activationS6 kinaseMEK activationBI-D1870Zebrafish modelCell motilityPrimary melanoma cellsGene expressionMicroarray analysisNovel roleSpreading cellsRSK1Melanoma invasionPromotes InvasionDifferential overexpressionNodular melanomaInvasionMolecular alterationsHistologic subtypeAngiolymphoid hyperplasia with eosinophilia.
Farhadian JA, Shvartsbeyn M, Meehan SA, Urbanek RW. Angiolymphoid hyperplasia with eosinophilia. Dermatology Online Journal 2015, 21 PMID: 26990330, DOI: 10.5070/d32112029531.Peer-Reviewed Original ResearchMeSH Keywords and ConceptsIgA vasculitis (Henoch-Schönlein purpura).
Farhadian JA, Castilla C, Shvartsbeyn M, Meehan SA, Neimann A, Pomeranz MK. IgA vasculitis (Henoch-Schönlein purpura). Dermatology Online Journal 2015, 21 PMID: 26990342, DOI: 10.5070/d32112029544.Peer-Reviewed Original ResearchCitationsMeSH Keywords and ConceptsConceptsIgA vasculitisAbdominal painDisease onsetUpper respiratory tract infectionImmunoglobulin A (IgA) vasculitisAcute abdominal painHenoch-Schönlein purpuraRespiratory tract infectionsCommon systemic vasculitisPalpable purpuraRenal involvementSystemic vasculitisAdult patientsRefractory casesTract infectionsClassic triadImmunosuppressive agentsInfluenza infectionBiopsy specimenVasculitisAmerican CollegeSmall arteriolesPurpuraPainFirst case
2013
Crystal deodorant‐induced axillary granulomatous dermatitis
Leventhal JS, Farhadian JA, Miller KE, Tlougan BE, Patel RR, Sanchez MR. Crystal deodorant‐induced axillary granulomatous dermatitis. International Journal Of Dermatology 2013, 53: e59-e60. PMID: 23621443, DOI: 10.1111/j.1365-4632.2012.05686.x.Peer-Reviewed Original ResearchAltmetric