Suspected coexistence of perianal necrotizing sweet syndrome in chronic myelomonocytic leukemia:A case report

BACKGROUND Chronic myelomonocytic leukemia(CMML)complicated with Sweet syndrome(SS)is a rare hematological neoplasm.However,cases of concomitant development of perianal necrotizing SS(NSS)have not been reported.CASE SUMMARY We report a case of a 49-year-old male patient who underwent sequential procedures for hemorrhoids and perianal abscess.He developed postoperative incision infection and was referred to the department where the authors work.Initially,perianal necrotizing fasciitis secondary to incision infection after perianal abscess surgery was suspected.Despite receiving antibiotic therapy and undergoing surgical debridement,deeper necrotic areas formed in the patient’s perianal wounds,accompanied by persistent high fever.Blood and fungal cultures yielded negative results.The final diagnosis was corrected to be CMML with suspected concomitant perianal NSS.CONCLUSION CMML with perianal NSS is a rare condition,often misdiagnosed as perianal abscess or perianal necrotizing fasciitis.Conventional antibiotic therapy and surgical debridement are ineffective in managing this condition.

Gene mutations in a patient with chronic myelomonocytic leukemia and changes upon progression to acute myeloid leukemia and during treatment

Objective Chronic myelomonocytic leukemia(CMML) has been categorized as an uncommon hematological malignancy with overlapping features of myelodysplastic syndromes(MDS) and myeloproliferative neoplasms that have an inherent risk of progressing to acute myeloid leukemia(AML). Methods This study presents a case of confirmed CMML combined with M protein, in which the molecular changes upon progression to AML and under decitabine(DAC) plus bortezomib therapy were reported by tracking variant allele frequency(VAF) of mutations in a series of bone marrow samples. Results First, variable sensitivity of clones was observed during DAC treatment, and incomplete mutation clearance may be associated with low overall response rate and unsustained response. Secondly, DAC cannot prevent the new genetic alterations and accumulation of genetic progression on treatment, leading to acute transformation. Finally, autoimmunity was found to have acted as an important pathogenetic factor, increasing the additive mutations that further drive the clonal evolution in CMML. Conclusion Overall, changes in mutations and clonal architecture during CMML progression or treatment are predictive of an early evaluation of therapeutic strategies in CMML.

Chronic myelomonocytic leukemia-associated pulmonary alveolar proteinosis:A case report and review of literature

BACKGROUND Pulmonary alveolar proteinosis(PAP)is a rare condition that can cause progressive symptoms including dyspnea,cough and respiratory insufficiency.Secondary PAP is generally associated with hematological malignancies including chronic myelomonocytic leukemia(CMML).To the best of our knowledge,this is the first reported case of PAP occurring secondary to CMML.CASE SUMMARY We report the case of a 63-year-old male who presented with a recurrent cough and gradually progressive dyspnea in the absence of fever.Based upon clinical symptoms,computed tomography findings,bone marrow aspiration,flow cytometry studies and cytogenetic analyses,the patient was diagnosed with PAP secondary to CMML.He underwent whole lung lavage in March 2016 to alleviate his dyspnea,after which he began combined chemotherapeutic treatment with decitabine and cytarabine.The patient died in January 2020 as a consequence of severe pulmonary infection.CONCLUSION This case offers insight regarding the mechanistic basis for PAP secondary to CMML and highlights potential risk factors.

Efficacy and safety of combined decitabine and ruxolitinib in the treatment of chronic myelomonocytic leukemia

Objective The aim of the study was to evaluate the clinical efficacy of decitabine(DEC)combined with ruxolitinib(RUX)in the treatment of chronic myelomonocytic leukemia(CMML).Methods The clinical characteristics of 12 patients with CMML were analyzed retrospectively and subsequent target sequencing was performed to investigate the efficacy of the combined treatment with DEC and RUX and the molecular signatures therein.Results Among the 12 cases,clinical improvement was observed in all patients(100%),spleen reduction was observed in six patients(67%),and hematologic improvement was observed in four patients(33%).In the CMML-1 group,the overall response was 50%(3/6),one case achieved complete response,one achieved bone marrow remission,and one achieved hematological improvement.In the CMML-2 group,the overall response was 17%(1/6),one case achieved complete response,four showed disease progression(PD),and one exhibited no response.As expected,ASXL1 mutation was predictive for the outcome of CMML(hazard ratio of 2.97,95%confidence interval of 1.21–7.06;P=0.02).Conclusion The use of DEC combined with RUX in the treatment of CMML effectively improved the clinical response and quality of life,especially for CMML-1 patients.Ongoing clinical trials will further evaluate the safety and efficacy of this novel therapeutic approach.

Chronic Myelomonocytic Leukemia with t （3; 9） （p21; p13） as a Sole Abnormal Appearance： One Case Report

Chronic myelomonocytic leukemia, （CMML） is a clinically rare chronic myeloid leukemia, with an incidence rate of about 1-2/ 100,000/year, and the age of the predominant cases is over 60 years. The median age of onset is 65-70 years, and the ratio of the incidence between male and female is about 1.5 ： 3.1. Specific etiological factors of the disease are not clear, but may be associated with the exposure to ionizing radiation,

Co-existing squamous cell carcinoma and chronic myelomonocytic leukemia with ASXL1 and EZH2 gene mutations:A case report

BACKGROUND Chronic myelomonocytic leukemia(CMML),a rare clonal hematopoietic stem cell disorder characterized by myelodysplastic syndrome and myeloproliferative neoplasms,has a generally poor prognosis,and easily progresses to acute myeloid leukemia.The simultaneous incidence of hematologic malignancies and solid tumors is extremely low,and CMML coinciding with lung malignancies is even rarer.Here,we report a case of CMML,with ASXL1 and EZH2 gene mutations,combined with non-small cell lung cancer(lung squamous cell carcinoma).CASE SUMMARY A 63-year-old male,suffering from toothache accompanied by coughing,sputum,and bloody sputum for three months,was given a blood test after experiencing continuous bleeding resulting from a tooth extraction at a local hospital.Based on morphological results,the patient was diagnosed with CMML and bronchoscopy was performed in situ to confirm the diagnosis of squamous cell carcinoma in the lower lobe of the lung.After receiving azacitidine,programmed cell death protein 1,and platinum-based chemotherapy drugs,the patient developed severe myelosuppression and eventually fatal leukocyte stasis and dyspnea.CONCLUSION During the treatment and observation of CMML and be vigilant of the growth of multiple primary malignant tumors.

Acute myelomonocytic leukemia and T-lymphoblastic lymphoma as simultaneous bilineage hematologic malignancy treated with decitabine:A case report

BACKGROUND Simultaneous bilineage hematologic malignancies are rare;however,several cases of acute myeloid leukemia(AML)and T-lymphoblastic lymphoma(T-LBL)cooccurrence have been reported.A standard treatment for simultaneous AML and T-LBL has not yet been established,and its prognosis is very poor.Further studies to develop standard treatments are required to increase patient survival rates.CASE SUMMARY A 69-year-old man complaining of pleuritic chest pain visited the emergency room.Computed tomography revealed multiple enlarged lymph nodes(LNs)in the neck and groin and pulmonary thromboembolism with pulmonary infarction.Furthermore,a peripheral blood smear performed due to leukocytosis revealed circulating blasts.Acute myelomonocytic leukemia(AMML)was diagnosed after bone marrow examination,and T-LBL positivity for terminal deoxynucleotidyl transferase,cluster of differentiation(CD)34,and CD4 was confirmed by cervical LN biopsy.Decitabine and dexamethasone were administered because he could not receive intensive chemotherapy due to poor performance status.Complete remission of AMML and T-LBL was achieved after 4 cycles of decitabine plus dexamethasone.CONCLUSION We report the therapeutic effect of decitabine,a hypomethylating agent(HMA),in patients with concurrent bilineage hematologic malignancies and suggest that further studies are required to evaluate the therapeutic effect of HMAs on both lymphoid and bilineage hematologic malignancies.

Initial Study on Immune Escape Mechanism of Mouse Acute Myelomonocytic Leukemic Cell Line WEHI-3

Objective： To investigate the expression of Fas, Fas ligand （FasL） and CD80 on the cell surface of mouse acute myelomonocytic leukemia cell line WEHI-3 and the function of FasL. Methods： The expression of Fas, FasL and CD80 was detected on WEHI-3 cell surface by flow cytometry. Simultaneously the function of FasL was determined by Thymidine （^3H-TdR） Incorporation. Results： The expression of CD80 and Fas on WEHI-3 cell surface was 5.06%±0.41% and 6.75%±2.31% （n=5） respectively, and the expression of FasL was up to 63.73%±5.23% （n=5）. The apoptotic rate of YAC-1 cells was 26%±4.5%, 35%±3.2% and 43%±2.7% （n=5） respectively when WEHI-3 （effector cell, E） and Fas^＋ YAC-1 cells （target cell, T） were cultured in the ratio of 3：1, 10：1 and 30：1. Conclusion： WEHI-3 cells express high FasL, low Fas and CD80, and can induce apoptosis of Fas^＋ YAC-1 cells.

Clinical manifestation of the SRSF2 gene mutation in Chinese patients with chronic myelomonocytic leukemia

Background Spliceosome mutations have been recently identified and associated with hematological malignancies. SRSF2, one of components of the splicing machinery, has a high mutation frequency during chronic myelomonocytic leukemia, according to previous reports. However, the relevance of this finding in Chinese populations remains unknown. Methods We recruited 50 Chinese patients with chronic myelomonocytic leukemia to analyze the state of SRSF2 and to assess the corresponding clinical features by polymerase chain reaction followed by direct sequencing. Results Ten of 50 patients （20%） harbored SRSF2 mutations, including five P95R, two 95H, and three P95L point mutations. The patient group was older than the wild type group （P 〈0.01）. No significant statistical differences were observed with regard to the other clinical characteristics （sex, peripheral blood count, serum lactate dehydrogenase, karyotype, World Health Organization classification, etc.） between these two groups. Two of the patients showed an early evolution to acute myeloid leukemia. Conclusions SRSF2 mutations are frequent in chronic myelomonocytic leukemia patients, but show a relatively lower incidence in Chinese patients. Moreover, the mutation can be related to old age and an unfavorable prognosis. Our results provide valuable insights for the development of a diagnostic marker, or for the identification of a therapeutic target for chronic myelomonocytic leukemia.

去甲基化药物在慢性粒单核细胞白血病中的临床疗效观察

目的:观察去甲基化药物在慢性粒单核细胞白血病(CMML)中的临床疗效及安全性。方法:回顾性分析2014年2月至2021年6月在河北医科大学第二医院确诊为CMML并应用去甲基化药物治疗的患者的临床资料、疗效指标、生存期及安全性。结果:共有25例CMML患者接受去甲基化药物治疗,18例以地西他滨为基础治疗,7例以阿扎胞苷为基础治疗。其中20例获得应答,7例获得完全缓解(CR),CR患者均以地西他滨为基础治疗,5例CR发生于治疗的前4个疗程。中位随访16.4(9.4-20.5)个月后,4例CR患者进展为急性髓系白血病。25例CMML患者的中位总生存期为17.4个月(95%CI:12.437-22.363)。按照MDAPS、CPSS、CPSS-mol、MMM预后积分系统分别对患者进行危险度分层,仅发现MDAPS预后积分系统不同危险度分层与生存期之间的差异有统计学意义。CMML患者应用去甲基化药物的常见不良反应包括感染、胃肠道反应、血液学毒性、皮肤过敏和肝功能损伤。所有患者给予相应的治疗后,症状均得到改善。结论:去甲基化药物对CMML患者治疗有效,且安全性良好。CR多发生于治疗的前4个疗程,对于无应答的患者,可应用去甲基化药物联合小剂量化疗。去甲基化药物可以延缓病情但并不能阻止CMML的疾病进展。

慢性粒-单核细胞白血病合并免疫性血小板减少症1例

慢性粒-单核细胞白血病(chronic myelomonocytic leukemia,CMML)合并免疫性血小板减少症(immune thrombocytopenia,ITP)十分罕见。该文报告1例采用维奈克拉联合瑞帕妥单抗(一种抗CD20单克隆抗体)及海曲泊帕治疗CMML合并ITP患者的临床资料。CMML和ITP的共存机制需要进一步明确。维奈克拉联合抗CD20单抗及血小板生成素受体激动剂可能是治疗该合并症的有效策略之一。

慢性粒单核细胞白血病合并自身免疫性疾病研究进展

慢性粒单核细胞白血病(chronic myelomonocytic leukemia,CMML)是一类以外周血单核细胞增多及骨髓异常增生为特征的克隆性造血干细胞疾病。CMML患者常合并自身免疫性疾病(autoimmune disease,AID),AID与CMML合并发生的机制尚不明确,给此类患者治疗的选择带来了一定挑战。已有研究提示合并AID对CMML患者的预后及治疗具有重要意义,本文就CMML患者合并AID的类型、可能发病机制、预后及相关治疗进展进行文献复习及综述。

非亲缘供者造血干细胞移植治疗JMML的临床疗效

目的评估非亲缘供者造血干细胞移植(URD-HSCT)治疗幼年粒单核细胞白血病(JMML)的临床疗效及安全性。方法回顾性分析2015年—2023年期间23例JMML移植患儿数据,中位移植年龄33(11-98)个月,PTPN11基因突变为主。供者选择HLA≥9/10位点相合的非亲缘供者。结果中位随访时间31(8-104)个月,输注CD34+中位数为4.8(1.3-12.5)×10^(6)/kg,23例均完全供者植入,粒细胞、血小板植入的中位时间分别为19天和13天,5年OS和LFS的统计预估值均为(91.1±6)%,无复发;Ⅱ度以上急性GVHD 7例(28%),Ⅲ-Ⅳ度仅1例;慢性GVHD 9例(39%),其中重度2例;移植相关死亡率8.9%。结论基于地西他滨的URD-HSCT方案治疗JMML临床疗效显著且安全,可作为JMML移植策略的优先推荐。

流式细胞分析在慢性粒-单核细胞白血病诊断中的价值探讨

慢性粒-单核细胞白血病(chronic myelomonocytic leukemia,CMML)是一种罕见的异质性血液系统恶性肿瘤,其重要特征之一是持续性单核细胞增多,这也是与其他疾病鉴别的关键,尤其需要与反应性单核细胞增多症进行鉴别。随着检验技术的不断进步以及对人类单核细胞亚群了解的增加,一些新的鉴别方法广泛应用,包括选取特定表面标志物、单核细胞亚群分型等方式。然而,通过流式细胞术选择特定表面标志物进行慢性粒-单核细胞白血病的诊断存在灵敏度低和特异性差的问题,而且至今尚未发现完全符合条件的表面标志物。对单核细胞亚群通过CD14/CD16分型定量,以单核细胞亚群占比进行慢性粒-单核细胞白血病的诊断与鉴别已经得到大量研究支持。但一些学者仍对这一方法在诊断中的准确性提出质疑,本文就该方面问题作一文献综述。

以全身紫红色结节为首发表现的慢性粒单核细胞白血病1例及文献复习

报告1例以全身紫红色结节为首发表现的慢性粒单核细胞白血病。患者女,75岁。因全身紫红色结节伴瘙痒10 d就诊。皮肤科检查:全身皮肤密集分布大量绿豆至黄豆大紫红色结节,边界清楚,部分融合,按压不褪色,局部皮温不高,无触痛,表面无鳞屑及水疱,部分表面可见溃疡、结痂,皮损分布以四肢为主。实验室及辅助检查:血常规中WBC计数30.0×10^(9)/L,单核细胞计数5.9×10^(9)/L,血小板计数17×10^(9)/L,红细胞计数1.8×10^(12)/L,血红蛋白65 g/L。骨髓象示早幼粒细胞比值占1.5%,原始血细胞占4%,原始单核细胞占0%,幼稚单核细胞占6%,成熟单核细胞占10%,成熟淋巴细胞占20.5%。骨髓免疫分型示淋巴细胞占3.12%,粒细胞占58.68%。流式细胞术检查:髓系原始细胞比例增高(2.13%),CD45表达减弱,表型异常;粒系以中幼粒细胞及之后阶段为主;嗜酸性粒细胞易见,嗜碱性粒细胞比例增高;单核细胞占有核细胞的25.81%,比例增高;红系CD71表达减弱。染色体荧光原位杂交(FISH):BCR-ABL190及BCR-ABL210融合基因均阴性。染色体核型分析:46,XX(7)。腹部超声示脂肪肝,胆囊壁毛糙。皮损组织病理检查:表皮局灶破溃和结痂,真皮乳头水肿,真皮全层血管周围及胶原间可见巢团状单核细胞、组织细胞及散在的嗜酸性粒细胞浸润,可见胶原纤维。诊断:慢性粒单核细胞白血病并累及皮肤。治疗:给予静脉滴注地西他滨35 mg/d;化疗5 d后皮损逐渐消退。13个月后随访,患者已死亡,但皮损未复发。

阿扎胞苷联合高三尖杉酯碱治疗老年慢性粒-单核细胞白血病的疗效和安全性分析

目的 评估阿扎胞苷联合高三尖杉酯碱治疗老年慢性粒-单核细胞白血病(CMML)的疗效和安全性。方法 纳入2018—2022年于我院确诊的40例老年CMML病人,按随机数表法分为试验组和对照组,每组20例。试验组接受阿扎胞苷联合高三尖杉酯碱治疗,对照组接受阿扎胞苷治疗,比较2组的疗效、安全性以及预后。结果 共36例病人入组,试验组19例,对照组17例。试验组总缓解率(ORR)高于对照组(84.2%比52.9%,P=0.041)。2组病人不良反应发生率比较,差异无统计学意义(P>0.05)。试验组病人中位生存时间为33.8个月,明显高于对照组中位生存时间(21.2个月)(P<0.05)。结论 阿扎胞苷联合高三尖杉酯碱方案治疗老年CMML安全有效。

多参数流式细胞术在慢性粒单核细胞白血病、骨髓增生异常综合症及急性单核细胞白血病免疫表型鉴别中的应用及其意义

本研究应用多参数流式细胞术分析慢性粒单核细胞白血病(CMML),骨髓增生异常综合症(DMS)以及急性单核细胞白血病(AML-M5b)的免疫表型特点,探究其在诊断及鉴别诊断上述疾病中的意义和价值。应用多参数流式细胞术比较分析14例CMML患者、48例MDS患者、46例AML-M5b患者及18例正常人骨髓标本的免疫分型特点。结果表明,CMML患者单核细胞比例明显高于MDS、AML-M5b患者及正常人骨髓(P<0.05),后3者之间无显著差别。MDS患者骨髓原始细胞比例明显高于正常骨髓标本(P<0.05),但与CMML患者无明显差别。AML-M5b患者骨髓成熟粒细胞比例较CMML、MDS患者及正常骨髓标本明显减低(P<0.05)。MDS、AML-M5b及CMML患者骨髓CD45/SSC特点与正常骨髓标本均存在一定差异。CMML患者骨髓具有CD2、CD56异常表达及CD14拖尾现象,与MDS、AML-M5b及正常骨髓标本相比差异显著(P<0.05)。MDS与CMML患者骨髓单核细胞CD15表达缺失或减低现象较正常骨髓标本及AML-M 5b患者显著,且CMML患者异常率高于MDS患者(P<0.05),两者粒细胞群均有显著CD13/CD11b/CD16表达规律异常现象,但两者间无显著差异。其他抗原表达呈不同程度异常,无统计学差异。结论 MDS、CMML及AML-M5b骨髓细胞免疫表型均具有各自的特点及不同程度的相似处。多参数流式细胞术综合分析其免疫表型,对于区分CMML、MDS以及AML-M5b具有重要鉴别意义。其中单核细胞比例增高,伴有CD2、CD56异常表达,CD14拖尾现象,CD15缺失或减低及成熟粒细胞CD13-CD11b-CD16表达规律异常,对CMML诊断具有重要意义。

异基因造血干细胞移植治疗慢性粒单核细胞白血病及幼年型粒单核细胞白血病

本研究探讨异基因造血干细胞移植治疗慢性粒单核细胞白血病(CMML)及幼年粒单核细胞型白血病(JMML)的疗效及其影响因素。对3例CMML及2例JMML患者接受异基因造血干细胞移植治疗的临床资料进行多参数分析。结果表明,造血干细胞在5例患者中均成功植入,除1例JMML死于移植后并发症外,余4例至今无病生存。移植前疾病负荷、染色体核型及II-IV度aGVHD的发生均对CMML的复发率或无病生存率有相关的影响;低剂量预处理方案优于清髓性预处理方案,而HLA的相合度及干细胞的来源均不影响总的生存率及无复发生存率,在JMML患者中脐带血造血干细胞移植的移植失败率明显高于骨髓或外周血造血干细胞移植;移植前脾脏的大小及是否行脾切除或者脾区照射对移植结果无影响,而移植年龄、GVHD的发生及HbF的水平对移植复发率均有重要意义。结论:异基因骨髓造血干细胞是治疗CMML及JMML的有效方法,但仍存在一系列问题需要解决。

幼年型粒单核细胞白血病的临床和治疗

目的探索幼年型粒单核细胞白血病(JMML)的早期临床、实验室特点,以提高诊断水平和治疗的有效性。方法分析17例JMML患儿的临床特征、外周血常规、单核细胞计数、血涂片,骨髓活检和/或骨髓穿刺的形态学和分子生物学,胎儿血红蛋白(HbF)和病毒抗原检测,诊断及治疗问题。结果17例患儿的年龄分布:2个月～5岁4个月,中位年龄14个月。临床表现:88.2%出现发热、面色苍白、咳嗽,76.5%胸片示支气管肺炎,皮肤出现丘疹58.8%,所有病例肝脾均肿大,其中≥5 cm者占52.9%,淋巴结肿大(浅表和深部)占82.4%。实验室:17例患儿外周血白细胞数中位值32.9×109/L、单核细胞绝对值中位值3.9×109/L,14/17例外周血涂片见髓系前体细胞,中位值28%,7例红系有病态造血,血红蛋白中位值88 g/L,血小板计数中位值33×109/L。骨髓活检和/或骨髓穿刺:原始、早幼粒/原幼单细胞数在5%～20%;14例作骨髓细胞免疫学检测,12例的免疫表型为MPO+、CD117+及其他的髓系标记,2例免疫表型为MPO-、CD14+、CD33+;14例进行细胞遗传分析,其中4例染色体单体改变依次为-8,+8q+、-6,+6q+、-20、-8;分子生物学检测bcr-abl基因阴性。HbF增高(中位值33%),病毒学检测EBV-IgM阳性7例、CMV-IgM阳性6例。结论JMML发病年龄以2岁以内多见,占60%。最初的诊断可类似ITP、病毒感染。JMML有效治疗很少,在缺乏相合供体情况下可选择联合化疗和诱导分化治疗。

急性白血病患者白血病细胞B7-H2的表达与预后关系的初步研究

目的研究急性白血病患者白血病细胞B7-H2的表达与预后的关系。方法收集47例初发的急性白血病[包括急性髓细胞白血病(AML)和急性淋巴细胞白血病(ALL)患者],应用流式细胞技术检测其白血病细胞上B7-H2的表达情况,分析所有白血病患者、AML患者及ALL患者预后因素与B7-H2表达的关系。另将47例患者分为B7-H2阳性率≥10%和B7-H2阳性率<10%两组,比较两组患者生存时间的差异。结果 47例急性白血病患者中,低危患者白血病细胞的B7-H2阳性率为0.04%±0.03%(n=24),中/高危患者为0.15%±0.07%(n=23,P=0.0015);在AML患者中,低危患者和中/高危患者白血病细胞B7-H2的阳性率为分别为0.05%±0.03%(n=16)和0.16%±0.09%(n=12,P=0.0412);在ALL患者中,低危患者和中/高危患者白血病细胞B7-H2的阳性率为分别为0.04%±0.03%(n=8)和0.15%±0.08%(n=11,P=0.0295)。47例白血病患者中,B7-H2阳性率≥10%的患者占25.53%,其中AML和ALL患者分别占21.42%(n=28)和31.57%(n=19);B7-H2阳性率≥10%的患者与B7-H2阳性率<10%的患者生存率有统计学差异(2χ=2.79,P=0.0453)。结论 B7-H2在急性白血病患者白血病细胞上有一定表达,并与预后密切相关。