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        Clinical and biological implications of driver mutations in myelodysplastic syndromes
        
        
            
        
    
        
                
            
    
    
        
        
    
                    
        
        The CSF3R T618I mutation causes a lethal neutrophilic neoplasia in mice that is responsive to therapeutic JAK inhibition
        
        
            
        
    
        
                
            
    
    
    
        
        
     
    
                    
                    
                
            
    
    
    
        
        
     
    
                    
                    
                
            
    
    
    
        
        
     
    
                    
                    
                
            
    
    
    
        
        
     
    
                     
    
                     
    
 
    
            
    
        
    
         
 
    
    
        
    
            
    
        
    
    
    
        
    
    
    
            
    
                    
 
    
    
 
    
    
        
    
    
    
            
        
 
    
    
 
    
    
        
    
    
    
            
        
            
    
        
        
    
             
            
             
            
             
        
    
 
    
    
 
    
    
        
    
    
    
            
    
                    
 
    
    
 
    
    
 
    
    
    
    
        
    Issue Archive
Table of Contents
INSIDE BLOOD
BLOOD WORK
REVIEW ARTICLE
REVIEW SERIES
HOW I TREAT
How I treat monoclonal gammopathy of renal significance (MGRS)
            Jean-Paul Fermand,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Frank Bridoux,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Robert A. Kyle,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Efstathios Kastritis,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Brendan M. Weiss,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Mark A. Cook,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Mark T. Drayson,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Angela Dispenzieri,on behalf of the International Kidney and Monoclonal Gammopathy Research Group,Nelson Leung,on behalf of the International Kidney and Monoclonal Gammopathy Research Group
            
        
    
            LYMPHOID NEOPLASIA
Detailed characterization of multiple myeloma circulating tumor cells shows unique phenotypic, cytogenetic, functional, and circadian distribution profile
            Bruno Paiva,Teresa Paino,Jose-Maria Sayagues,Mercedes Garayoa,Laura San-Segundo,Montserrat Martín,Ines Mota,María-Luz Sanchez,Paloma Bárcena,Irene Aires-Mejia,Luis Corchete,Cristina Jimenez,Ramon Garcia-Sanz,Norma C. Gutierrez,Enrique M. Ocio,Maria-Victoria Mateos,Maria-Belen Vidriales,Alberto Orfao,Jesús F. San Miguel
            
        
    
            Indolent T-cell lymphoproliferative disease of the gastrointestinal tract
            Anamarija M. Perry,Roger A. Warnke,Qinglong Hu,Philippe Gaulard,Christiane Copie-Bergman,Serhan Alkan,Huan-You Wang,Jason X. Cheng,Chris M. Bacon,Jan Delabie,Erik Ranheim,Can Kucuk,XiaoZhou Hu,Dennis D. Weisenburger,Elaine S. Jaffe,Wing C. Chan
            
        
    
            MYELOID NEOPLASIA
        
        Clinical and biological implications of driver mutations in myelodysplastic syndromes
        
        
            
        
                    
                        CME
                    
        
            
    
        
            Elli Papaemmanuil,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Moritz Gerstung,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Luca Malcovati,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Sudhir Tauro,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Gunes Gundem,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Peter Van Loo,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Chris J. Yoon,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Peter Ellis,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,David C. Wedge,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Andrea Pellagatti,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Adam Shlien,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Michael John Groves,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Simon A. Forbes,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Keiran Raine,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Jon Hinton,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Laura J. Mudie,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Stuart McLaren,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Claire Hardy,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Calli Latimer,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Matteo G. Della Porta,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Sarah O’Meara,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Ilaria Ambaglio,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Anna Galli,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Adam P. Butler,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Gunilla Walldin,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Jon W. Teague,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Lynn Quek,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Alex Sternberg,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Carlo Gambacorti-Passerini,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Nicholas C. P. Cross,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Anthony R. Green,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Jacqueline Boultwood,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Paresh Vyas,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Eva Hellstrom-Lindberg,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,David Bowen,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Mario Cazzola,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Michael R. Stratton,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium,Peter J. Campbell,on behalf of the Chronic Myeloid Disorders working group of the International Cancer Genome Consortium
            
        
    
            
        
        The CSF3R T618I mutation causes a lethal neutrophilic neoplasia in mice that is responsive to therapeutic JAK inhibition
        
        
            
        
                    
                        Brief Report
                    
        
            
    
        
            Angela G. Fleischman,Julia E. Maxson,Samuel B. Luty,Anupriya Agarwal,Lacey R. Royer,Melissa L. Abel,Jason D. MacManiman,Marc M. Loriaux,Brian J. Druker,Jeffrey W. Tyner
            
        
    
            PLATELETS AND THROMBOPOIESIS
Highly electronegative LDL from patients with ST-elevation myocardial infarction triggers platelet activation and aggregation
            Hua-Chen Chan,Liang-Yin Ke,Chih-Sheng Chu,An-Sheng Lee,Ming-Yi Shen,Miguel A. Cruz,Jing-Fang Hsu,Kai-Hung Cheng,Hsiu-Chuan Bonnie Chan,Jonathan Lu,Wen-Ter Lai,Tatsuya Sawamura,Sheng-Hsiung Sheu,Jeng-Hsien Yen,Chu-Huang Chen
            
        
    
            TRANSPLANTATION
Amino acid substitution at peptide-binding pockets of HLA class I molecules increases risk of severe acute GVHD and mortality
            Joseph Pidala,Tao Wang,Michael Haagenson,Stephen R. Spellman,Medhat Askar,Minoo Battiwalla,Lee Ann Baxter-Lowe,Menachem Bitan,Marcelo Fernandez-Viña,Manish Gandhi,Ann A. Jakubowski,Martin Maiers,Susana R. Marino,Steven G. E. Marsh,Machteld Oudshoorn,Jeanne Palmer,Vinod K. Prasad,Vijay Reddy,Olle Ringden,Wael Saber,Stella Santarone,Kirk R. Schultz,Michelle Setterholm,Elizabeth Trachtenberg,E. Victoria Turner,Ann E. Woolfrey,Stephanie J. Lee,Claudio Anasetti
            
        
    
            VASCULAR BIOLOGY
Rasip1 regulates vertebrate vascular endothelial junction stability through Epac1-Rap1 signaling
            Christopher W. Wilson,Leon H. Parker,Christopher J. Hall,Tanya Smyczek,Judy Mak,Ailey Crow,George Posthuma,Ann De Mazière,Meredith Sagolla,Cecile Chalouni,Philip Vitorino,Merone Roose-Girma,Søren Warming,Judith Klumperman,Philip S. Crosier,Weilan Ye
            
        
    
            CORRESPONDENCE
CONTINUING MEDICAL EDUCATION (CME) QUESTIONS
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            Cover Image
        
        
Cover Image
            The image shows the cranial vasculature (green) and red blood cells (red) from a 48-hour-old zebrafish embryo injected with rasip1 anti-sense morpholino oligonucleotide. Circulating red blood cells can be seen within the lumen of blood vessels. Accumulation of extravascular red blood cells indicates hemorrhage due to vascular instability. See the article by Wilson et al on page 3678.
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