The term congenital neutropenia encompasses a family of neutropenic disorders, both permanent and intermittent, severe (<0.5 G/l) or mild (between 0.5-1.5 G/l), which may also affect other organ systems such as the pancreas, central nervous system, heart, muscle and skin. Neutropenia can lead to life-threatening pyogenic infections, acute gingivostomatitis and chronic parodontal disease, and each successive infection may leave permanent sequelae. The risk of infection is roughly inversely proportional to the circulating polymorphonuclear neutrophil count and is particularly high at counts below 0.2 G/l.When neutropenia is detected, an attempt should be made to establish the etiology, distinguishing between acquired forms (the most frequent, including post viral neutropenia and auto immune neutropenia) and congenital forms that may either be isolated or part of a complex genetic disease.Except for ethnic neutropenia, which is a frequent but mild congenital form, probably with polygenic inheritance, all other forms of congenital neutropenia are extremely rare and have monogenic inheritance, which may be X-linked or autosomal, recessive or dominant.About half the forms of congenital neutropenia with no extra-hematopoetic manifestations and normal adaptive immunity are due to neutrophil elastase (ELANE) mutations. Some patients have severe permanent neutropenia and frequent infections early in life, while others have mild intermittent neutropenia.Congenital neutropenia may also be associated with a wide range of organ dysfunctions, as for example in Shwachman-Diamond syndrome (associated with pancreatic insufficiency) and glycogen storage disease type Ib (associated with a glycogen storage syndrome). So far, the molecular bases of 12 neutropenic disorders have been identified.Treatment of severe chronic neutropenia should focus on prevention of infections. It includes antimicrobial prophylaxis, generally with trimethoprim-sulfamethoxazole, and also granulocyte-colony-stimulating factor (G-CSF). G-CSF has considerably improved these patients' outlook. It is usually well tolerated, but potential adverse effects include thrombocytopenia, glomerulonephritis, vasculitis and osteoporosis. Long-term treatment with G-CSF, especially at high doses, augments the spontaneous risk of leukemia in patients with congenital neutropenia.
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机译:先天性中性粒细胞减少症包括永久性和间歇性,严重(<0.5 G / l)或轻度(0.5-1.5 G / l)的中性粒细胞减少症,也可能影响其他器官系统,例如胰腺,中枢神经系统,心脏,肌肉和皮肤。中性粒细胞减少症可导致威胁生命的化脓性感染,急性牙龈炎和慢性牙周疾病,每次连续感染都可能留下永久性后遗症。感染的风险与循环中的多形核中性粒细胞计数大致成反比,尤其是在低于0.2 G / l的计数中尤其高。当检测到中性粒细胞减少时,应尝试确定病因,以区分获得性形式(最常见的是包括病毒性中性粒细胞减少和自身免疫性中性粒细胞减少)以及可能是孤立的或复杂遗传疾病一部分的先天性形式。除种族中性粒细胞减少症(一种常见但轻度的先天性形式,可能具有多基因遗传性)外,其他所有形式的先天性中性粒细胞减少症极少见且具有单基因遗传,可能是X连锁或常染色体遗传,隐性或显性遗传的。约一半形式的先天性中性粒细胞减少症没有血细胞外表现且正常的适应性免疫力是由于中性粒细胞弹性蛋白酶(ELANE)突变引起的。一些患者患有严重的永久性中性粒细胞减少症,并在生命早期频繁感染,而其他患者则患有轻度的间歇性中性粒细胞减少症。先天性中性粒细胞减少症也可能与多种器官功能障碍有关,例如Shwachman-Diamond综合征(与胰腺功能不全有关)和糖原Ib型贮积病(与糖原贮积综合征相关)。到目前为止,已经确定了12种中性粒细胞减少症的分子基础,严重慢性中性粒细胞减少症的治疗应着重于感染的预防。它包括抗菌预防,通常与甲氧苄氨嘧啶,磺胺甲基异恶唑一起使用,以及粒细胞集落刺激因子(G-CSF)。 G-CSF大大改善了这些患者的视线。通常耐受性良好,但潜在的不良反应包括血小板减少症,肾小球肾炎,血管炎和骨质疏松症。 G-CSF的长期治疗,尤其是大剂量的长期治疗,会增加先天性中性粒细胞减少症患者的自发性白血病风险。
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