Acute intermittent porphyria in adults: a clinical case

Kubanskii nauchnyi meditsinskii vestnik Pub Date : 2022-01-25 DOI:10.25207/1608-6228-2022-29-1-96-107

M. Barabanova, Yu. A. Tsymbal, E. Y. Efimenko, T. A. Petropavlovskaia, I. Velichko

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Abstract

Background. Porphyria unites genetic pathologies related to abnormal haem (an intermediate product of haemoglobin metabolism) synthesis and its toxic products accumulation in human body. Symptoms can vary, from photosensitivity, skin rashes and chronic abdominal pain towards partial or complete paralysis and acute psychosis. This metabolic disorder is diagnosed with molecular genetic and laboratory biosample tests. Drug therapy aims at reducing toxic metabolites concentration in patient’s blood.Clinical Case Description. A 28-yo female patient had an acute atypical porphyria attack with a later onset of neurovisceral manifestations (acute abdominal pain, tachycardia) progressing post-drug-treatment into acute sensorimotor polyneuropathy with ﬂaccid, predominantly proximal, hands-prevalent tetraparaesis. Biochemical urine tests at the National Research Center for Hematology (by 30.06.2020) revealed porphobilinogen 55.3 mg/L at norm <3. Vital indications required an urgent haem arginate pathogenetic therapy (Normosang) in a 4-day course of 3 mg/kg/day drop infusion. The recommended course was well tolerated. Drug therapy and rehabilitation entailed a positive dynamics of restoring limb muscle strength towards an almost easy getting-up from chair and bed, and skin lightening. The patient was discharged on day 20 with diagnosis: “Acute intermittent porphyria. Axonal-demyelinating sensorimotor polyneuropathy. Severe ﬂaccid asymmetric predominantly proximal hands-prevalent tetraparaesis. Subacute course, stabilisation phase. Condition after one course of haem arginate pathogenetic therapy (Normosang) at 3 mg/kg/day”. A resident haematologist surveillance was recommended, with a routine referral for inpatient examination and treatment at the Department of Orphan Diseases of the National Research Center for Hematology, Ministry of Health of Russia.Conclusion. Porphyria is relatively rarely diagnosed, about 12 cases per 100,000 people. The symptoms variety and nonspeciﬁcity conduce to a low detection rate, and untimely diagnoses can entail severe clinical manifestations, including lethal outcomes.

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成人急性间歇性卟啉1例

背景卟啉综合征是与血红素（血红蛋白代谢的中间产物）合成异常及其毒性产物在人体内积累有关的遗传病理。症状各不相同，从光敏性、皮疹和慢性腹痛到部分或完全瘫痪和急性精神病。这种代谢紊乱是通过分子遗传学和实验室生物样本测试诊断出来的。药物治疗旨在降低患者血液中有毒代谢产物的浓度。临床病例描述。一名28岁的女性患者发生急性非典型卟啉症发作，随后出现神经内脏表现（急性腹痛、心动过速），药物治疗后发展为急性感觉运动性多发性神经病，并伴有以近端为主的四肢畸形。国家血液学研究中心的生化尿液测试（截至2020年6月30日）显示，卟啉原55.3 mg/L，正常值<3。生命体征需要紧急的血红素精氨酸病因治疗（Normosang），为期4天，每天滴注3 mg/kg。推荐的疗程耐受性良好。药物治疗和康复需要恢复肢体肌肉力量，使其几乎可以轻松地从椅子和床上爬起来，并使皮肤变亮。患者于第20天出院，诊断为：“急性间歇性卟啉症。轴索性脱髓鞘感觉运动性多发性神经病。严重不对称，主要是近端手，普遍存在四肢瘫痪。亚急性病程，稳定期。在3 mg/kg/天的精氨酸血症病因治疗（Normosang）一个疗程后病情恶化”。建议进行住院血液学家监测，并定期转诊到俄罗斯卫生部国家血液学研究中心孤儿疾病科进行住院检查和治疗。结论：卟啉病相对较少被诊断，约每10万人中有12例。症状的多样性和非特异性导致检测率低，诊断不及时可能导致严重的临床表现，包括致命后果。

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