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沧州市中心医院滤泡淋巴瘤专家

简介:

沧州市中心医院始建于1898年,是国家首批三级甲等综合性医院,拥有丰富的医疗资源和专业的医疗团队。医院在滤泡淋巴瘤等恶性肿瘤治疗方面具有显著优势,设有沧州市肿瘤诊疗中心,为患者提供全面的诊疗服务。医院心血管内科、肿瘤外科等专业在滤泡淋巴瘤治疗方面积累了丰富经验,成功开展多项高精尖技术。医院秉承“患者至上”的理念,致力于为滤泡淋巴瘤患者提供高质量的医疗服务,助力患者重获健康。沧州市中心医院,守护您的健康,共创美好未来。滤泡淋巴瘤是起源于淋巴造血系统的恶性肿瘤,主要表现为无痛性淋巴结肿大,肝脾肿大,全身各组织器官均可受累,伴发热、盗汗、消瘦、瘙痒等全身症状。,病因不清。一般认为,可能和基因突变,以及病毒及其他病原体感染、放射线、化学药物,合并自身免疫病等有关。,淋巴,1.放射治疗 某些类型的淋巴瘤早期可以单纯放疗。放疗还可用于化疗后巩固治疗及移植时辅助治疗。 2.化学药物治疗 淋巴瘤化疗多采用联合化疗,可以结合靶向治疗药物和生物制剂。近年来,淋巴瘤的化疗方案得到了很大改进,很多类型淋巴瘤的生存期都得到了很大提高。 3.骨髓移植 对60岁以下患者,能耐受大剂量化疗的中高危患者,可考虑进行自体造血干细胞移植。部分复发或骨髓侵犯的年轻患者还可考虑异基因造血干细胞移植。 4.手术治疗 仅限于活组织检查或并发症处理;合并脾机能亢进而无禁忌证,有切脾指征者可以切脾,以提高血象,为以后化疗创造有利条件。,慢性淋巴结炎,无,1.血常规及血涂片 血常规一般正常,可合并慢性病贫血;HL可以出现PLT增多、WBC增多、嗜酸性粒细胞增多;侵袭性NHL侵犯骨髓可出现贫血、WBC及PLT减少,外周血可出现淋巴瘤细胞。 2.骨髓涂片及活检 HL罕见骨髓受累。NHL侵犯骨髓,骨髓涂片可见淋巴瘤细胞,细胞体积较大,染色质丰富,灰蓝色,形态明显异常,可见“拖尾现象”;淋巴瘤细胞≥20%为淋巴瘤白血病;骨髓活检可见淋巴瘤细胞聚集浸润。部分患者骨髓涂片可见噬血细胞增多及噬血现象,多见于T细胞NHL。 3.血生化 LDH增高与肿瘤负荷有关,为预后不良的指标。HL可有ESR增快,ALP增高。 4.脑脊液检查 中高度侵袭性NHL临床Ⅲ/Ⅳ期患者可能出现中枢神经系统受累,或有中枢神经系统症状者,需行脑脊液检查,表现为脑脊液压力增高,生化蛋白量增加,常规细胞数量增多,单核为主,病理检查或流式细胞术检查可发现淋巴瘤细胞。 5.组织病理检查 HL的基本病理形态学改变是在以多种炎症细胞的混合增生背景中见到诊断性的R-S细胞及其变异型细胞。免疫组化特征:经典型CD15+,CD30+,CD25+;结节淋巴细胞为主型CD19+,CD20+,EMA+,CD15-,CD30-。NHL淋巴结或组织病理见正常淋巴结或组织结构破坏,肿瘤细胞散在或弥漫浸润,根据不同的病理类型有各自独特的病理表现和免疫表型。 6.TCR或IgH基因重排 可阳性。 诊断,。

赵素敏 主任医师

阴道炎,早孕,先兆流产,妊娠期糖尿病,甲状腺功能减退,胎儿生长受限,胚胎停育,早产及妊娠高血压疾病,宫颈机能不全,前置胎盘等产科合并症的诊断及治疗。

好评 99%
接诊量 1.8万
平均等待 15分钟
擅长:阴道炎,早孕,先兆流产,妊娠期糖尿病,甲状腺功能减退,胎儿生长受限,胚胎停育,早产及妊娠高血压疾病,宫颈机能不全,前置胎盘等产科合并症的诊断及治疗。
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吴昱 副主任医师

小儿腹泻、小儿腹痛、小儿便秘、厌食症、喂养困难、小儿肥胖、营养不良、微量营养素缺乏、黄疸、肝病、儿童甲亢、甲减、青春发育异常、矮小症。

好评 100%
接诊量 247
平均等待 1小时
擅长:小儿腹泻、小儿腹痛、小儿便秘、厌食症、喂养困难、小儿肥胖、营养不良、微量营养素缺乏、黄疸、肝病、儿童甲亢、甲减、青春发育异常、矮小症。
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翟福瑞 主治医师

治疗外阴瘙痒分泌物异常导致的各种阴道炎如霉菌、细菌、滴虫等,同时擅长治疗异常子宫出血,月经失调,妇科内分泌疾病,内膜息肉,宫颈病变的诊断及治疗,宫颈HPV感染的治疗及阴道镜检查,超声下的输卵管造影,宫腔镜检查等。

好评 100%
接诊量 505
平均等待 30分钟
擅长:治疗外阴瘙痒分泌物异常导致的各种阴道炎如霉菌、细菌、滴虫等,同时擅长治疗异常子宫出血,月经失调,妇科内分泌疾病,内膜息肉,宫颈病变的诊断及治疗,宫颈HPV感染的治疗及阴道镜检查,超声下的输卵管造影,宫腔镜检查等。
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崔红帅 主治医师

擅长新生儿以及婴儿喂养问题。对儿童呼吸道、慢性咳嗽、各种肺炎以及小儿急救经验丰富。

好评 99%
接诊量 644
平均等待 30分钟
擅长:擅长新生儿以及婴儿喂养问题。对儿童呼吸道、慢性咳嗽、各种肺炎以及小儿急救经验丰富。
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杨柳 主治医师

不明原因发热,病毒性肝炎,结核病,麻疹,水痘,腮腺炎等传染性疾病。

好评 99%
接诊量 6121
平均等待 30分钟
擅长:不明原因发热,病毒性肝炎,结核病,麻疹,水痘,腮腺炎等传染性疾病。
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马艳菲 主治医师

血液科常见病多发病及疑难病的诊治 贫血,再生障碍性贫血,纯红细胞再生障碍,多发性骨髓瘤,淋巴瘤,白血病,白细胞减少,血小板减少,血小板增多,出血,红细胞增多,地中海贫血,溶血性贫血,血友病,缺铁性贫血,营养不良,慢性粒细胞白血病,慢性淋巴细胞白血病,紫癜。 血常规解读、血常规、白细胞 红细胞、血小板、出血点、瘀斑、鼻子出血、乏力、贫血、白细胞高等等,血液异常,血象异常,血异常

好评 100%
接诊量 142
平均等待 15分钟
擅长:血液科常见病多发病及疑难病的诊治 贫血,再生障碍性贫血,纯红细胞再生障碍,多发性骨髓瘤,淋巴瘤,白血病,白细胞减少,血小板减少,血小板增多,出血,红细胞增多,地中海贫血,溶血性贫血,血友病,缺铁性贫血,营养不良,慢性粒细胞白血病,慢性淋巴细胞白血病,紫癜。 血常规解读、血常规、白细胞 红细胞、血小板、出血点、瘀斑、鼻子出血、乏力、贫血、白细胞高等等,血液异常,血象异常,血异常
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张仁亮 主治医师

擅长对各科常见病多发病(如感冒、咳嗽、慢性胃炎、头痛等)做出中西医全面系统调理治疗。尤其擅长中医治疗各类男科疾病:阳痿、早泄、男性不育、男性乳房疾病、阴茎、睾丸及前列腺增生疾病,感染后男性功能障碍、血精、精液不液化、尿频尿急、男子男性疲劳症各种男科疾病。

好评 100%
接诊量 12
平均等待 15分钟
擅长:擅长对各科常见病多发病(如感冒、咳嗽、慢性胃炎、头痛等)做出中西医全面系统调理治疗。尤其擅长中医治疗各类男科疾病:阳痿、早泄、男性不育、男性乳房疾病、阴茎、睾丸及前列腺增生疾病,感染后男性功能障碍、血精、精液不液化、尿频尿急、男子男性疲劳症各种男科疾病。
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张西凯 副主任医师

擅长:儿科呼吸系统疾病、神经系统疾病、消化系统疾病、泌尿系统疾病、血液系统疾病、儿科中毒、儿科休克、儿科呼衰

好评 99%
接诊量 3993
平均等待 15分钟
擅长:擅长:儿科呼吸系统疾病、神经系统疾病、消化系统疾病、泌尿系统疾病、血液系统疾病、儿科中毒、儿科休克、儿科呼衰
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王庆 副主任医师

白血病,再生障碍性贫血,多发性骨髓瘤,淋巴瘤,骨髓增生异常综合征,贫血,血小板减少症及各种出凝血疾病

好评 100%
接诊量 1
平均等待 -
擅长:白血病,再生障碍性贫血,多发性骨髓瘤,淋巴瘤,骨髓增生异常综合征,贫血,血小板减少症及各种出凝血疾病
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于静 主任医师

长期从事妇科肿瘤、妇科门诊各种疾病及疑难杂症的诊治。擅长各种妇科内分泌疾病的诊断治疗,如闭经、功血、性发育异常、围绝经期相关疾病、不孕不育诊治及辅助生育技术,尤其擅长妇科各种疾病的宫腔镜、腹腔镜治疗、各种阴式手术以及女性内外生殖器整形手术。

好评 99%
接诊量 320
平均等待 -
擅长:长期从事妇科肿瘤、妇科门诊各种疾病及疑难杂症的诊治。擅长各种妇科内分泌疾病的诊断治疗,如闭经、功血、性发育异常、围绝经期相关疾病、不孕不育诊治及辅助生育技术,尤其擅长妇科各种疾病的宫腔镜、腹腔镜治疗、各种阴式手术以及女性内外生殖器整形手术。
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患友问诊

患者因眼部受汗刺激出现不适,持续一天,考虑可能由淋巴滤泡引起,寻求医生建议。患者男性36岁
56
2024-10-31 05:36:59
我有扁桃体发炎和喉咙小泡泡,已经两天了,想知道如何治疗?患者男性25岁
7
2024-10-31 05:36:59
我父亲被诊断为滤泡性淋巴瘤1级,医生建议放疗17次,但我担心他体质和免疫力不佳,是否能够承受放疗?患者男性53岁
56
2024-10-31 05:36:59
老人新冠阳性,体温38.5度,伴有咳嗽、咽干咽痛和头痛,如何用药?患者男性86岁
52
2024-10-31 05:36:59
滤泡淋巴瘤老人,缺白蛋白,咨询是否可以用蛋白粉补充。
27
2024-10-31 05:36:59
63岁滤泡性淋巴瘤患者在化疗中,新冠阳性,免疫力低下,想获取辉瑞药物,如何操作?患者女性63岁
63
2024-10-31 05:36:59
发热37.5度,头疼,长期服用恩替卡韦,三项抗体阳性,滤泡淋巴瘤治疗后感染新冠。患者女性34岁
33
2024-10-31 05:36:59
滤泡淋巴瘤患者出现下午肚胀,担心与病情有关,想了解原因和处理方法。患者男性61岁
14
2024-10-31 05:36:59
72岁高血压患者出现低血压,需进一步检查?患者男性72岁
35
2024-10-31 05:36:59
滤泡性淋巴瘤是一种慢性B细胞非霍奇金淋巴瘤,患者担心其是否可以治愈并寻求治疗建议。患者男性59岁
6
2024-10-31 05:36:59

科普文章

以下内容来源于新英格兰医学杂志。

Presentation of Case

Dr. Christine M. Parsons (Medicine): A 75-year-old woman was evaluated at this hospital because of arthritis, abdominal pain, edema, malaise, and fever.

Three weeks before the current admission, the patient noticed waxing and waning “throbbing” pain in the right upper abdomen, which she rated at 9 (on a scale of 0 to 10, with 10 indicating the most severe pain) at its maximal intensity. The pain was associated with nausea and fever with a temperature of up to 39.0°C. Pain worsened after food consumption and was relieved with acetaminophen. During the 3 weeks before the current admission, edema developed in both legs; it had started at the ankles and gradually progressed upward to the hips. When the edema began to affect her ambulation, she presented to the emergency department of this hospital.

A review of systems that was obtained from the patient and her family was notable for intermittent fever, abdominal bloating, anorexia, and fatigue that had progressed during the previous 3 weeks. The patient reported new orthopnea and nonproductive cough. Approximately 4 weeks earlier, she had had diarrhea for several days. During the 6 weeks before the current admission, the patient had lost 9 kg unintentionally; she also had had pain in the wrists and hands, 3 days of burning and dryness of the eyes, and diffuse myalgias. She had not had night sweats, dry mouth, jaw claudication, vision changes, urinary symptoms, or oral, nasal, or genital ulcers.

The patient’s medical history was notable for multiple myeloma (for which treatment with thalidomide and melphalan had been initiated 2 years earlier and was stopped approximately 1 year before the current admission); hypothyroidism; chikungunya virus infection (diagnosed 7 years earlier); seropositive erosive rheumatoid arthritis affecting the hands, wrists, elbows, and shoulders (diagnosed 3 years earlier); vitiligo; and osteoarthritis of the right hip, for which she had undergone arthroplasty. Evidence of gastritis was reportedly seen on endoscopy that had been performed 6 months earlier. Medications included daily treatment with levothyroxine and acetaminophen and pipazethate hydrochloride as needed for cough. The patient consumed chamomile and horsetail herbal teas. She had no known allergies to medications, but she had been advised not to take nonsteroidal antiinflammatory drugs after her diagnosis of multiple myeloma.

Approximately 5 months before the current admission, the patient had emigrated from Central America. She lived with her daughter and grandchildren in an urban area of New England. She had previously worked in health care. She had no history of alcohol, tobacco, or other substance use. There was no family history of cancer or autoimmune, renal, gastrointestinal, pulmonary, or cardiac disease.

On examination, the temporal temperature was 37.1°C, the heart rate 106 beats per minute, the blood pressure 152/67 mm Hg, and the oxygen saturation 100% while the patient was breathing ambient air. She had a frail appearance and bitemporal cachexia. The weight was 41 kg and the body-mass index (the weight in kilograms divided by the square of the height in meters) 15.2. Her dentition was poor; most of the teeth were missing, caries were present in the remaining teeth, and the mucous membranes were dry. She had abdominal tenderness on the right side and mild abdominal distention, without organomegaly or guarding. Bilateral axillary lymphadenopathy was palpable. Infrequent inspiratory wheezing was noted.

The patient had swan-neck deformity, boutonnière deformity, ulnar deviation, and distal hyperextensibility of the thumbs (Fig. 1). Subcutaneous nodules were observed on the proximal interphalangeal joints of the second and third fingers of the right hand and on the proximal interphalangeal joint of the fourth finger of the left hand. Synovial thickening of the metacarpophalangeal joints of the second fingers was noted. There was mild swelling and tenderness of the wrists. She had pain with flexion of the shoulders and right hip, and there was subtle swelling of the shoulders and right knee. Pitting edema (3+) and vitiligo were noted on the legs. No sclerodactyly, digital pitting, telangiectasias, appreciable calcinosis, nodules, nail changes (including pitting), or tophi were present. The remainder of the examination was normal.

Figure 1

Photograph of the Hands.

The blood levels of glucose, alanine aminotransferase, aspartate aminotransferase, bilirubin, globulin, lactate, lipase, magnesium, and phosphorus were normal, as were the prothrombin time and international normalized ratio; other laboratory test results are shown in Table 1. Urinalysis showed 3+ protein and 3+ blood, and microscopic examination of the sediment revealed 5 to 10 red cells per high-power field and granular casts. Urine and blood were obtained for culture. An electrocardiogram met (at a borderline level) the voltage criteria for left ventricular hypertrophy.

Table 1
Laboratory Data.

Dr. Rene Balza Romero: Computed tomography (CT) of the chest, abdomen, and pelvis, performed after the intravenous administration of contrast material, revealed scattered subcentimeter pulmonary nodules (including clusters in the right middle lobe and patchy and ground-glass opacities in the left upper lobe), trace pleural effusion in the left lung, coronary and valvular calcifications, and trace pericardial effusion, ascites, and anasarca. The scans also showed slight enlargement of the axillary lymph nodes (up to 11 mm in the short axis) bilaterally and a chronic-appearing compression fracture involving the T12 vertebral body.

Dr. Parsons: Morphine and lactated Ringer’s solution were administered intravenously. On the second day in the emergency department (also referred to as hospital day 2), the blood levels of haptoglobin, folate, and vitamin B12 were normal; other laboratory test results are shown in Table 1. A rapid antigen test for malaria was positive. Wright–Giemsa staining of thick and thin peripheral-blood smears was negative for parasites; the smears also showed Döhle bodies and basophilic stippling. Antigliadin antibodies and anti–tissue transglutaminase antibodies were not detected. Tests for hepatitis A IgG and hepatitis C antibodies were positive. Tests for hepatitis B core and surface antibodies were negative. A test for human immunodeficiency virus type 1 (HIV-1) and type 2 (HIV-2) was negative.

Findings on abdominal ultrasound imaging performed on the second day (Fig. 2A and 2B) were notable for a small volume of ascites and kidneys with echogenic parenchyma. Ultrasonography of the legs showed no deep venous thrombosis. An echocardiogram showed normal ventricular size and function, aortic sclerosis with mild aortic insufficiency, moderate tricuspid regurgitation, a right ventricular systolic pressure of 39 mm Hg, and a small circumferential pericardial effusion. Intravenous hydromorphone was administered, and the patient was admitted to the hospital.

Figure 2

Imaging Studies of the Abdomen and Hands.

On the third day (also referred to as hospital day 3), nucleic acid testing for cytomegalovirus, Epstein–Barr virus, and hepatitis C virus was negative, and a stool antigen test for Helicobacter pylori was negative. An interferon-γ release assay for Mycobacterium tuberculosis was also negative. Oral acetaminophen and ivermectin and intravenous hydromorphone and furosemide were administered.

Dr. Balza Romero: Radiographs of the hands (Fig. 2C through 2F) showed joint-space narrowing of both radiocarpal joints and proximal interphalangeal erosions involving both hands. Radiographs of the shoulders showed arthritis of the glenohumeral joint and alignment suggestive of a tear of the right rotator cuff. A radiograph of the pelvis showed diffuse joint-space narrowing of the left hip, without osteophytosis, and an intact right hip prosthesis.

Dr. Parsons: Diagnostic tests were performed, and management decisions were made.

Differential Diagnosis

Dr. Beth L. Jonas: This patient is a 75-year-old woman who recently emigrated from Central America. She presented to this hospital with a multisystem disease involving the respiratory, gastrointestinal, renal, and musculoskeletal systems. Her medical history is notable for seropositive erosive rheumatoid arthritis and multiple myeloma, which had been treated with melphalan and thalidomide. Relevant clinical features on presentation include unintended weight loss and cachexia, axillary lymphadenopathy, serositis, cytopenia in two cell lines, hypocomplementemia, and elevated serum free kappa and lambda light-chain levels (with a normal free light-chain ratio) with no monoclonal spike. The white-cell count was elevated, but she had no eosinophilia. CT images of the chest showed scattered subcentimeter pulmonary nodules. With respect to the patient’s anemia, no schistocytes were present, the haptoglobin level was normal, and the iron studies were unremarkable. These findings, in combination with the elevated ferritin level, indicate anemia of chronic inflammation. The renal findings are most salient in the context of the patient’s hypertension, anasarca, elevated cystatin C level, active urinary sediment with proteinuria in the nephrotic range, and small, echogenic kidneys on ultrasonography.
In constructing a differential diagnosis, I will consider medication use, cancer, infectious disease, and autoimmune disease. Medications can be eliminated as the cause of this patient’s illness, since she was taking only levothyroxine, acetaminophen, and the antitussive agent pipazethate.

Cancer

The patient has a history of multiple myeloma, which may manifest with a multisystem disease involving the kidneys, but serum protein electrophoresis showed no monoclonal protein. Given the presence of nephrotic syndrome in the context of multiple myeloma, systemic immunoglobulin light-chain amyloidosis would be highest on the differential diagnosis with respect to cancer; however, the patient’s normal light-chain ratio makes this diagnosis unlikely. The development of myeloid neoplasms, such as acute myeloid leukemia, myelodysplastic syndromes, and myeloproliferative neoplasms, is important to consider in the context of previous treatment with alkylating agents, 1 which this patient had received. However, the peripheral-blood smear showed no findings that would indicate a hematologic cancer, and such a diagnosis would not explain the patient’s acute kidney injury with nephrotic-range proteinuria.

Infectious Disease

Several features of this patient’s case warrant special consideration, including her history of immunosuppression due to rheumatoid arthritis and to previously treated myeloma, along with the fact that she had emigrated from Central America, where certain infections may be prevalent. Infection with hepatitis A virus, hepatitis B virus, hepatitis C virus, HIV-1 and HIV-2, cytomegalovirus, Epstein–Barr virus, H. pylori, and M. tuberculosis can be ruled out on the basis of laboratory studies. A rapid antigen test for plasmodium species was reported to be positive, but this assay has a known cross-reactivity with rheumatoid factor. 2 Moreover, the thick and thin peripheral-blood smears were negative. Thus, malaria would be an unlikely diagnosis.
The patient has a history of infection with chikungunya virus, an arbovirus transmitted by a mosquito vector that has been responsible for large epidemics in the Americas since 2013. 3 Acute symptoms include fever, rash, arthralgia, and myalgia. The development of a chronic arthritis that may meet the classification criteria for rheumatoid arthritis, as defined by the American College of Rheumatology and the European Alliance of Associations for Rheumatology, has been reported in up to 60% of patients infected with chikungunya virus. 4,5 In the context of this discussion, I considered whether chikungunya virus infection could be the cause of this patient’s symptoms, since this infection occurred before the diagnosis of rheumatoid arthritis. However, the degree of erosion and loss of joint space that was visible on radiographs would be most unusual for arthritis associated with chikungunya virus infection and would not explain the renal manifestations.
Strongyloidiasis is a helminth infection (caused by Strongyloides stercoralis) that is widespread in developing countries. Infection usually occurs through contact with soil, and most affected persons are asymptomatic. However, in immunosuppressed persons, strongyloides hyperinfection syndrome or a disseminated infection can develop as a consequence of accelerated autoinfection. 6 The clinical presentation of strongyloides hyperinfection syndrome can include gastrointestinal symptoms (diarrhea, constipation, nausea, or vomiting), respiratory symptoms (cough, dyspnea, or wheezing), and rash due to migration of larvae through the subcutaneous tissues. Of note, only a minority of patients present with eosinophilia. Several case reports describe the development of nephrotic-range proteinuria, thrombotic microangiopathy, and IgA vasculitis in patients with strongyloides hyperinfection syndrome. 7-9 However, strongyloidiasis would not explain this patient’s cytopenias and hypocomplementemia.

Autoimmune Disease

The patient has a 3-year history of rheumatoid arthritis, although her clinical features of swan-neck deformity, boutonnière deformity, and joint instability suggest a longer duration of disease. We do not know whether she had received previous treatment with disease-modifying antirheumatic drugs or biologic agents, but the possible use of such treatments may be a consideration with respect to her progression of disease and overall degree of immunosuppression. The blood levels of rheumatoid factor and anti–cyclic citrullinated peptide antibodies were elevated, and radiographs of the hands showed erosive disease, although there was a relative paucity of metacarpophalangeal findings. A review of systems was negative for dry mouth, but her physical examination showed poor dentition and dry mouth — findings that make secondary Sjögren’s syndrome a consideration.
Renal disease can occur in patients with Sjögren’s syndrome. The two most typical presentations are tubulointerstitial nephritis and, less commonly, nephritic syndrome (membranoproliferative glomerulonephritis related to cryoglobulinemia). Tubulointerstitial nephritis may manifest with renal disease of varying severity, usually with a bland urinary sediment and often with abnormalities of tubular function such as distal renal tubular acidosis. Membranoproliferative glomerulonephritis caused by cryoglobulinemia is the most common glomerular disease associated with Sjögren’s syndrome. Although nephrotic-range proteinuria can occur with Sjögren’s syndrome, it is relatively uncommon. 10 Renal disease is uncommon in patients with rheumatoid arthritis and is usually related to coexisting cardiovascular conditions. Medications used in the treatment of autoimmune disease — mainly nonsteroidal antiinflammatory drugs — may be associated with renal disease, but I would not expect the presence of an active urinary sediment, as was seen in this patient.
Amyloid A (AA) amyloidosis, a condition that is rare in the era of aggressive management of rheumatoid arthritis, has been described in patients with severe, long-standing seropositive erosive rheumatoid arthritis. Serum amyloid A (SAA) is a protein that is produced in the liver in response to chronic inflammation associated with interleukin-1, interleukin-6, and tumor necrosis factor α (TNF-α) in the context of chronic infections, autoimmune disease (classically rheumatoid arthritis), autoinflammatory disease, and cancers including renal cell carcinoma and non-Hodgkin’s lymphoma. 11 Signs and symptoms of AA amyloidosis are related to the deposition of the protein in organs, and patients often present with multisystem signs and symptoms. The kidney is the organ that is most often affected, but deposition can occur in the heart, gastrointestinal tract, nervous system, musculoskeletal system, and lungs. Proteinuria is the first clinical manifestation in almost 95% of patients with AA amyloidosis, and 50% of affected patients present with nephrotic syndrome. 12 The urinary sediment is generally bland, and complement levels in the blood are normal. AA amyloidosis remains on the differential diagnosis in this patient, but it would not completely explain her renal disease.

Hypocomplementemia

The key to this case is understanding the cause of this patient’s hypocomplementemia. Hypocomplementemia can be due to decreased complement production in the context of liver disease, congenital complement deficiency, or increased complement consumption resulting from activation of the innate immune system. This patient has no history of chronic liver disease and her laboratory test results indicated good hepatic synthetic function. Classical complement deficiency (including C4 deficiency) that begins early in life is associated with autoimmune disease, and early C3 deficiency is characterized by severe pyogenic infections. It would be unusual for a patient of this age to be deficient in both C3 and C4 without earlier clinical consequences. I therefore concluded that the hypocomplementemia in this case was related to complement consumption.
Rheumatic diseases that may be associated with prominent renal manifestations include antineutrophil cytoplasmic antibody–associated vasculitis, systemic sclerosis with renal crisis, cryoglobulinemic vasculitis, antiglomerular basement membrane disease, and systemic lupus erythematosus (SLE). Of those conditions, SLE would be the most likely to be manifested by an active urinary sediment and nephrotic-range proteinuria with consumption of both C3 and C4 in the context of fever, thrombocytopenia, and serositis. This patient’s fever, thrombocytopenia, and serositis also fit with this diagnosis. 13
Because the patient has long-standing seropositive erosive rheumatoid arthritis, a diagnosis of AA amyloidosis is strongly suspected. Moreover, given the presence of thrombocytopenia, hypocomplementemia, and an active urinary sediment, I would recommend a kidney biopsy to evaluate for lupus nephritis and AA amyloidosis.

Dr. Beth L. Jonas’s Diagnosis

Overlap syndrome of rheumatoid arthritis and systemic lupus erythematosus with amyloid A amyloidosis.

Pathological Discussion

Dr. Claire Trivin-Avillach: Testing for autoimmune antibodies was performed. A test for antinuclear antibodies was positive at a titer of 1:5120 with a homogeneous pattern, and a test for anti–double-stranded DNA antibodies was positive at a titer of 1:2560.
The diagnostic procedure in this case was a core-needle biopsy of the kidney. Examination of the specimen with light microscopy revealed 20 glomeruli, 45% of which were globally sclerosed, along with fibrosis involving approximately 60% of the interstitium and tubular atrophy. Diffusely enlarged glomeruli with thickened capillary walls and an expanded mesangium were weakly positive on periodic acid–Schiff staining; the glomeruli stained pale blue on Masson’s trichrome staining. Congo red staining revealed metachromatic salmon-colored deposition involving the glomeruli, the blood-vessel walls, and the interstitium, which was associated with apple-green birefringence when viewed under polarized light (Fig. 3A). In addition, mesangial and endocapillary hypercellularity was identified in approximately 30% of the nonsclerosed glomeruli and was associated with karyorrhexis (Fig. 3B). One cellular crescent was also detected. These features are characteristic of active proliferative glomerulonephritis.
Figure 3
Biopsy Specimen of the Kidney.
Immunofluorescence microscopy revealed prominent granular staining for IgG (4+), IgM (4+), C3 (3+), C1q (3+), IgA (1+), kappa (3+), and lambda (3+) along the glomerular basement membranes and within the mesangium, as well as focal granular deposits of IgG and C3 along the tubular basement membrane (Fig. 3C and 3D). Additional immunofluorescence studies showed strong positivity (4+) for SAA within the glomeruli, the blood-vessel walls, and the interstitium (Fig. 3E), whereas staining for beta2-microglobulin, transthyretin, and apolipoprotein A1 was faint.
Electron microscopy revealed the presence of subendothelial and mesangial electron-dense deposits (with no substructure identified) adjacent to randomly arranged fibrils (measuring 8.2 to 10.6 nm in diameter) within the glomerular basement membranes and the mesangium (Fig. 3F). Glomerular endothelial cells appeared reactive and contained tubuloreticular inclusions, features that were suggestive of interferon-mediated activation.
The findings on Congo red staining were characteristic of amyloidosis with typical birefringent material. The strong positivity of SAA within the deposits as compared with the faint staining of other reactants identified the type of amyloid as SAA, which is consistent with the patient’s history of rheumatoid arthritis. The biopsy also showed an immune complex–mediated proliferative glomerulonephritis with a “full house” pattern (defined as positivity for the three immunoglobulin classes IgG, IgM, and IgA and the two complement components C3 and C1q, in reference to the “full house” hand in a poker game). Immune complex–mediated proliferative glomerulonephritis has been reported in patients with rheumatoid arthritis who were receiving anti–TNF-α therapy, 14 which was not the case in this patient. The positive test for hepatitis C antibodies prompted consideration of hepatitis C–related membranoproliferative glomerulonephritis. However, taken together, the negative nucleic acid test for hepatitis C virus, the full house pattern on immunofluorescence, the tubular basement membrane deposits, and the positive test for anti–double-stranded DNA antibodies favor a diagnosis of lupus nephritis of at least class III (defined as focal proliferative glomerulonephritis), according to the criteria of the International Society of Nephrology and the Renal Pathology Society, superimposed on AA amyloidosis.

Pathological Diagnosis

Proliferative lupus nephritis of International Society of Nephrology and Renal Pathology Society class III, superimposed on amyloid A amyloidosis.

Discussion of Management

Dr. Pui W. Cheung: On the basis of the finding of echogenic kidneys on ultrasonography and the findings of extensive interstitial fibrosis and tubular atrophy on kidney biopsy, we know that this patient has advanced chronic kidney disease that is unlikely to be reversible. The patient is also noted to have a markedly lower glomerular filtration rate (GFR) than that predicted by the blood creatinine level owing to the presence of cachexia, and this is substantiated by the cystatin C–based GFR and a 24-hour creatinine clearance of 22 ml per minute per 1.73 m2 of body-surface area. The typical induction therapy for stage III or IV lupus nephritis consists of high-dose glucocorticoids and either mycophenolate mofetil or cyclophosphamide. Other reasonable alternatives for initial therapy include mycophenolate mofetil in combination with either a calcineurin inhibitor or belimumab, or cyclophosphamide in combination with belimumab. 15 Hydroxychloroquine is also recommended as part of the therapy, since it has shown benefits in improving the response to treatment and reducing disease flare. 16 Mycophenolate mofetil and cyclophosphamide have similar efficacy with respect to clinical response, which includes a reduction in proteinuria and either an improvement in renal function or stabilization of renal function; the risks of infections and adverse events associated with these medications are also similar. 17,18
Given the severity of the lupus nephritis with overlying AA amyloidosis from active rheumatoid arthritis, the treatment options proposed were high-dose glucocorticoids and rituximab with either mycophenolate mofetil or cyclophosphamide. 19 After discussions with multidisciplinary consultants from rheumatology, infectious diseases, and nephrology, lingering concerns were raised about infection and patient frailty; ultimately, the decision was made to initiate high-dose glucocorticoid therapy in combination with mycophenolate mofetil, rituximab, and hydroxychloroquine.
The patient’s mycophenolate mofetil dose regimen was inconsistent owing to gastrointestinal side effects, and the treatment was eventually withheld because of pancytopenia and fever. Unfortunately, her kidney function worsened, and renal replacement therapy was initiated within 3 weeks after the start of the induction therapy. The cause of her renal failure was thought to be disease progression, compounded by hemodynamically mediated tubular injury in the context of infection. While the administration of mycophenolate mofetil was stopped, treatment with rituximab was continued, with slow tapering of the glucocorticoid dose at the direction of the rheumatologist. She remained dependent on dialysis and was deemed to have end-stage kidney disease after 3 months of dialysis.
Dr. Lisa G. Criscione-Schreiber: The patient has SLE with nephritis, seropositive erosive rheumatoid arthritis, and systemic AA amyloidosis. AA amyloidosis is rare owing to the availability of effective therapies for rheumatoid arthritis and is managed through aggressive treatment of inflammation due to rheumatoid arthritis. Reports addressing the management of rheumatoid arthritis–induced AA amyloidosis generally cite stability of end-organ damage caused by AA amyloid as evidence of effective management of the condition (through treatment of the inflammation of rheumatoid arthritis). Methotrexate, the cornerstone of treatment for rheumatoid arthritis, is contraindicated in this case owing to the presence of kidney disease. The alkylating agent cyclophosphamide has been reported to be effective for the treatment of AA amyloidosis from rheumatoid arthritis 20 and has known efficacy in patients with lupus nephritis, both of which make it a viable treatment option. Rituximab has also been reported to be effective for managing rheumatoid arthritis–induced AA amyloidosis, 21 is approved for the treatment of rheumatoid arthritis, and is used for manifestations of SLE, including thrombocytopenia and nephritis. Although anti–TNF-α agents, abatacept, and Janus kinase inhibitors are reported to be effective for the treatment of AA amyloidosis in patients with rheumatoid arthritis, 22 recent publications have coalesced on the ability of anti–interleukin-6 therapy to block interleukin-6–induced hepatic production of SAA. 23-25
The overlap of seropositive erosive rheumatoid arthritis and SLE (sometimes termed “rhupus”) usually resembles rheumatoid arthritis more than SLE; manifestations include thrombocytosis, leukocytosis, an elevated erythrocyte sedimentation rate, an elevated blood level of C-reactive protein, and the presence of marginal erosions on radiographs. 26 In contrast, SLE without seropositive erosive rheumatoid arthritis characteristically manifests with thrombocytopenia, leukopenia, and an elevated erythrocyte sedimentation rate but usually not an elevated C-reactive protein level; in addition, nonerosive inflammatory arthritis with reversible deformities is commonly observed. This patient had a mixed laboratory profile, on the basis of the results of antinuclear antibody and anti–double-stranded DNA antibody tests. The challenge of treating an overlap syndrome of rheumatoid arthritis and SLE is choosing disease-modifying antirheumatic drugs that are effective and safe in both conditions. This patient’s most severe disease manifestation is lupus nephritis; therefore, the treatment regimen must target nephritis along with the AA amyloidosis and inflammatory arthritis.
As noted earlier, current induction therapy for lupus nephritis includes either mycophenolate mofetil or cyclophosphamide. Mycophenolate mofetil may provide inadequate treatment of the rheumatoid arthritis and amyloidosis, whereas cyclophosphamide would treat the lupus nephritis, has possible efficacy for treatment of the AA amyloidosis, and would treat the rheumatoid arthritis. Rituximab could be added to cyclophosphamide or mycophenolate mofetil to treat the rheumatoid arthritis and resultant AA amyloidosis and could also possibly help treat the lupus nephritis. The addition of anti–interleukin-6 therapy to mycophenolate mofetil or cyclophosphamide is an intriguing option that may effectively treat the rheumatoid arthritis and subsequent AA amyloidosis. The addition of belimumab to mycophenolate mofetil or cyclophosphamide has been reported to improve renal response in patients with lupus nephritis, 27 as has the addition of voclosporin to mycophenolate mofetil. 28 However, belimumab is ineffective for the treatment of rheumatoid arthritis, and voclosporin has not been studied in patients with rheumatoid arthritis or in those with a GFR of 45 milliliters per minute or less. The high-dose glucocorticoids that are used in induction therapy for lupus nephritis will effectively manage this patient’s inflammatory arthritis and probably also the subsequent AA amyloidosis. Finally, it is important that every patient with lupus nephritis receive hydroxychloroquine, which improves the treatment response to induction therapy. 29

Follow-up

Dr. Parsons: The patient’s hospital course was further complicated by suspected immune-mediated thrombocytopenia, for which she received intravenous immune globulin. Her pancytopenia and arthritis ultimately abated. Unfortunately, she did not have renal recovery and continues to receive hemodialysis. After a prolonged hospital course, she was discharged home.

Final Diagnosis

Overlap syndrome of rheumatoid arthritis and systemic lupus erythematosus complicated by proliferative lupus nephritis, superimposed on amyloid A amyloidosis.

泌乳素轻度偏高与多种因素相关。
 
从生理因素来看,日常活动就有影响,像剧烈运动、体力劳动后,泌乳素会出现轻度上升。睡眠也对其有作用,睡眠不足或睡眠质量差可能导致泌乳素轻度升高,而在入睡后的一段时间内,泌乳素分泌会自然增加。另外,处于妊娠期和哺乳期的女性,身体需要为泌乳做准备和进行哺乳活动,泌乳素会升高,这是正常的生理反应。
 
精神因素也不容忽视。长期处于紧张、焦虑、压力大的精神状态下,比如工作压力巨大的上班族或临近重大考试的学生,会引起神经调节功能紊乱,从而导致泌乳素分泌轻度异常。
 
再者是饮食因素。如果经常食用一些含激素类食物,特别是含有较高雌激素的食物,可能会刺激垂体分泌泌乳素。同时,过度饮酒、高蛋白高脂肪饮食也可能和泌乳素轻度偏高有一定关联。
 
某些药物也会造成泌乳素升高。常见的如抗精神病药物、抗抑郁药物、降压药等,这些药物在治疗疾病的同时,可能会对内分泌系统产生副作用,使泌乳素水平轻度上升。
 
最后是疾病因素。一些下丘脑疾病、垂体微腺瘤等会影响泌乳素的正常分泌,但在疾病初期,可能仅表现为泌乳素轻度偏高,还可能有甲状腺功能减退症,因为甲状腺激素分泌不足会反馈影响下丘脑 - 垂体轴,从而导致泌乳素升高。
男性泌乳素轻度偏高与多种因素有关。
 
在生理方面,首先是性生活因素。性生活不规律或过度手淫,可能引起短暂的泌乳素升高。此外,男性乳头受到刺激,比如摩擦、挤压或外伤等,会向大脑传递信号,使泌乳素分泌增加。年龄也是一个因素,随着男性年龄增长,身体机能变化,泌乳素水平可能出现一定程度的自然波动,有可能轻度偏高。
 
疾病因素也很关键。下丘脑 - 垂体疾病会对泌乳素的调控产生影响,垂体瘤是其中较为常见的原因。当垂体瘤存在时,可能压迫或刺激泌乳素细胞,使其分泌增加。另外,甲状腺功能减退症会引起甲状腺激素水平降低,通过下丘脑 - 垂体 - 甲状腺轴的反馈调节机制,促使下丘脑分泌更多的促甲状腺激素释放激素,而这种激素可能刺激垂体分泌泌乳素。慢性肾功能不全也会导致泌乳素升高,因为肾功能异常时,身体对泌乳素的代谢和排泄能力下降,使体内泌乳素水平上升。
 
药物的副作用也不容忽视。多巴胺受体拮抗剂,如抗精神病药物中的氯丙嗪、奋乃静等,通过阻断多巴胺受体,抑制多巴胺对泌乳素分泌的抑制作用,从而导致泌乳素升高。某些降压药,如利血平,会干扰多巴胺的储存和释放,也可能引起泌乳素轻度偏高。
 
最后,精神和生活习惯也会影响泌乳素水平。长期的精神紧张、焦虑、抑郁等精神状态,会干扰下丘脑的神经调节功能,引起泌乳素分泌异常。不良的生活习惯,如长期熬夜、过度饮酒、暴饮暴食等,可能通过影响身体的内分泌和代谢功能,间接导致泌乳素轻度偏高。
#不孕症 妇科炎症#妇科用药#真菌性阴道炎
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思恩腾瑞贝安医用妇科凝胶使用方法

1、清洗双手及外阴;

2、取下无菌盖套(上盖);

3、抠出密封盖(下盖);

4、将无菌套作为推杆使用;

5、轻缓放入阴道挤出敷料;

6、使用枕头垫高臀部,平躺15~30分钟。

#复诊HPV及TCT#妊娠合并人乳头瘤病毒(HPV)感染#人乳头瘤病毒感染
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思恩腾瑞贝安抗人乳头瘤病毒(HPV)敷料使用方法

1、清洗双手及外阴;

2、取下无菌盖套(上盖);

3、抠出密封盖(下盖);

4、将无菌套作为推杆使用;

5、轻缓放入阴道挤出敷料;

6、使用枕头垫高臀部,平躺15~30分钟。

#复诊HPV及TCT#妊娠合并人乳头瘤病毒(HPV)感染#人乳头瘤病毒感染
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思恩腾瑞贝安 抗HPV 生物蛋白敷料 使用方法

1、清洗双手及外阴;

2、取下无菌盖套(上盖);

3、抠出密封盖(下盖);

4、将无菌套作为推杆使用;

5、轻缓放入阴道挤出敷料;

6、使用枕头垫高臀部,平躺15~30分钟。

1️⃣什么是 发热?

通常儿童腋温≥37.5℃或肛温≥38℃为发热。

以腋温为准,37.5~38℃为低热,38.1~38.9℃为中度发热,39~40.9℃为高热,≥41℃为超高热。

2️⃣体温怎么测?

测量工具:水银温度计、电子温度计、红外温度计等。

测量方法(以水银温度计为例):擦干腋窝汗液→水银温度计消毒→将汞柱甩到35℃以下→将水银头放在腋窝中→上臂紧压腋窝5到10分钟→捏住水银温度计尾端,取出读数。

3️⃣怎么护理?

发热患儿往往经历体温上升期→高热期→体温下降期的过程。

体温上升期可能出现四肢冰凉、畏寒、寒战,这时需要适当保温;

高热期全身达到高峰,开始出汗,需要停止一切保温措施,甚至需要适当的减少衣物以便散热,千万不能盖厚被捂热。

体温下降期可能因大汗浸湿衣物,应注意更换衣物,避免受凉再次感冒。

4️⃣发热对机体有什么影响?

发热对机体的影响利弊并存,可造成食欲减退、营养消耗增加、水电解质平衡紊乱甚至热性惊厥等,但中等程度的发热也可增强某些免疫细胞的功能,提高宿主的防御能力。

5️⃣什么时候使用退热药?

≥2月龄儿童腋温≥38.2℃,或因发热导致不舒适和情绪低落时。

6️⃣用什么退热药?

目前儿童推荐使用的退热药有两种:布洛芬和对乙酰氨基酚。

7️⃣有什么副作用?

给药剂量适当时,布洛芬和对乙酰氨基酚不良反应较少。

对乙酰氨基酚偶见皮疹、白细胞减少等;

布洛芬一般为轻度的胃肠不适,偶有皮疹、耳鸣、头痛等。

超量使用退热药则可能导致严重的肝损害、肾损害或严重的心脏毒性、消化道出血、严重的皮肤反应等。

8️⃣布洛芬和对乙酰氨基酚选哪一种?

通常情况下,布洛芬和对乙酰氨基酚在疗效方面相当、安全性相似。

①注意年龄:<2月龄禁用;≥2月龄且<6月龄,使用对乙酰氨基酚;≥6月龄使用布洛芬或对乙酰氨基酚。

②非必要不使用,若必须要使用,这些情况优先选择布洛芬:肝功能不好、蚕豆病(胡豆黄)、关节炎等;这些情况优先选择对乙酰氨基酚:年龄小、腹泻、脱水、水痘、心功能不好等。

9️⃣还有哪些方法可以帮助退热?

改善舒适度:如温水外敷额头、温水浴、适当减少穿着的衣物、退热贴、退热毯、降低环境温度等。

不推荐加酒精沐浴、冰水灌肠等方法。

此外,还应注意摄入更多水份,清淡饮食,注意休息,避免过多刺激。

若孩子年龄小,或反复发热大于3天无好转,或反复发热超过5天,或持续高热至下一次用退热药前,或出现面色苍白、皮肤黏膜发绀、呼吸困难、小便明显减少、拒绝交流互动等情况需要立即到医院就诊。

需要强调一下:

️退热的目的不是一味地追求恢复正常体温,而主要是为了减轻发热所致的不适,改善舒适度。

️一般情况下,不推荐布洛芬与对乙酰氨基酚联合或交替使用。

#黑色棘皮症
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肥胖人脖子黑可能有以下原因:

一、黑棘皮病

1. 发病机制:肥胖人群体内胰岛素水平相对较高,胰岛素抵抗较为明显。高胰岛素血症会刺激皮肤角质细胞和纤维母细胞增殖,导致皮肤过度角化和色素沉着,从而引起黑棘皮病,表现为脖子等皮肤褶皱处发黑。

2. 特点:黑棘皮病除了颈部皮肤发黑外,还可能伴有皮肤增厚、粗糙等症状。病变皮肤常呈现出天鹅绒样或乳头瘤样外观。

二、摩擦和污垢堆积

1. 原因:肥胖人群的颈部相对较粗,皮肤褶皱较多,容易出汗且通风不良。在日常活动中,颈部皮肤之间的摩擦增加,加上汗液、灰尘等容易在褶皱处堆积,久而久之可能导致皮肤颜色变深。

2. 特点:这种情况下的皮肤发黑通常比较表浅,经过清洁和护理后可能会有所改善。

三、内分泌及代谢因素

1. 解释:肥胖会引起体内内分泌和代谢的紊乱。一些激素水平的变化可能影响皮肤的色素代谢,导致色素沉着在颈部等部位。例如,肾上腺皮质激素分泌异常等情况可能与皮肤色素沉着有关。

2. 表现:这种由于内分泌及代谢因素导致的脖子黑,通常是全身代谢紊乱的一个表现之一,可能同时伴有其他症状,如月经不调、多毛等。

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