Dear Editor,
We read with interest the report in the present Journal of Edington M. et al [1] titled “Prescribing lessons from an ocular chemical injury: Vitaros inadvertently dispensed instead of VitA-POS”.
Erectile disfunction drugs play a role increasing levels of cyclic guanosine monophosphate (cGMP) with subsequent effects on nitric-oxide release. This condition can lead to acute angle-closure glaucoma (AACG) in case of anatomical predisposition. AACG is an ophthalmic emergency, it can lead to irreversible blindness if not identified and treated immediately and precipitating factors include certain drugs as nitrates, bronchodilators, cough mixtures, cold and flu medication, antidepressants, antihistamines and anticonvulsants [2]. Furthermore, a precedent case of AACG following sildenafil citrated therapy is also described [3].
We would like underline that this situation could lead to more serious effects, that only the mild chemical ocular injury, in presence of ophthalmic structural diseases.

References:
1. Edington M, Connolly J, Lockington D. Prescribing lessons from an ocular chemical injury: Vitaros inadvertently dispensed instead of VitA-POS. BMJ Case Rep. 2018 Dec 3;11(1). doi: 10.1136/bcr-2018-227468.
2. Murray D. Emergency management: angle-closure glaucoma. Community Eye Health. 2018;31(103):64.
3. Ramasamy B, Rowe F, Nayak H, Peckar C, Noonan C. Acute angle-closure glaucoma following sildenafil citrate-aided sexual intercourse. Acta Ophthalmol Scand. 2007; 85: 229-230.

We wish to share our clinical experience and support the importance of long term monitoring of thyroid function in patients with central congenital hypothyroidism caused by maternal thyrotoxicosis. This is a case series of three infants with prolonged hypothyroxinaemia unrelated to the initial management of neonatal Graves’ disease (NGD). In contrast to the minimal antenatal care reported in the case report. mothers of all infants in our case series had antenatal diagnosis of Graves’ disease with appropriate management and close follow up for signs of fetal hyperthyroidism. All infants were diagnosed with NGD within two weeks of birth with two infants being commenced on antithyroid medication for 2-4 weeks as they were symptomatic with NGD.

With resolution of NGD, thyroid function tests were monitored with subsequent hypothyroxinaemia noted between 4-8 weeks of age. Having confirmed persistent hypothyroxinaemia, all infants were commenced on thyroxine (4-10mcg/kg/day) with regular follow up of their thyroid function tests.

The development of hypothyroxinaemia after initial treatment of NGD is uncommon however has been described previously (1). In most cases, NGD remits by 3-12 weeks once maternal antibodies are cleared (2, 3). Early transient hypothyroxinaemia in infants of poorly controlled maternal Graves’ is well reported due to high circulating antibodies particularly in the third trimester (1, 4). Postulated mechanisms include suppression of the pituitary-thyroid axis due to fetal hyperthyroxinaemia caused by transplacental transfer of thyroxine in untreated hyperthyroid mothers or of thyroid-stimulating immunoglobulin from the mother (4, 5). It is not surprising the longstanding effects of poorly controlled maternal Graves’ disease given the early effects on thyroid function, with TSH receptors becoming responsive to TSH and to TSH-receptor antibodies around 20 weeks (6) and the hypothalamic-pituitary-thyroid axis continues to mature from the second half of gestation until one to two months postnatal.

The role of thyrotropin receptor antibodies has also been reported in the ‘switching’ between hypothyroidism to hyperthyroidism or vice versa. McLachlan et al described that varying concentration and affinities of thyroid stimulating versus blocking antibodies and immunological effect associated with the primary disease itself could contribute to ‘switching’ (7). Recovery of TSH levels tend to be delayed and has been reported to take up to 3-19 months in childhood Graves and up to 3¼ years in treated NGD (4).

Hypothyroxinaemia post initial management of NGD is an uncommon entity in addition to the rare background occurrence of NGD, but requires early recognition so that appropriate treatment may be instigated. There are known risk factors that predict the development of NGD but from this case series, there were no obvious factors that suggested the subsequent development of hypothyroxinaemia. It raises the importance of frequent clinical monitoring of growth and development supported by ongoing screening of TFTs in NGD.

References
1. Papendieck P, Chiesa A, Prieto L, Gruneiro-Papendieck L. Thyroid disorders of neonates born to mothers with Graves' disease. J Pediatr Endocrinol Metab. 2009;22(6):547-53.
2. Levy-Shraga Y, Tamir-Hostovsky L, Boyko V, Lerner-Geva L, Pinhas-Hamiel O. Follow-up of newborns of mothers with Graves' disease. Thyroid : official journal of the American Thyroid Association. 2014;24(6):1032-9.
3. Kamishlian A, Matthews N, Gupta A, Filipov P, Maclaren N, Anhalt H, et al. Different outcomes of neonatal thyroid function after Graves' disease in pregnancy: patient reports and literature review. J Pediatr Endocrinol Metab. 2005;18(12):1357-63.
4. Matsuura N, Harada S, Ohyama Y, Shibayama K, Fukushi M, Ishikawa N, et al. The mechanisms of transient hypothyroxinemia in infants born to mothers with Graves' disease. Pediatric research. 1997;42(2):214-8.
5. Higuchi R, Kumagai T, Kobayashi M, Minami T, Koyama H, Ishii Y. Short-term hyperthyroidism followed by transient pituitary hypothyroidism in a very low birth weight infant born to a mother with uncontrolled Graves' disease. Pediatrics. 2001;107(4):E57.
6. Polak M, Le Gac I, Vuillard E, Guibourdenche J, Leger J, Toubert ME, et al. Fetal and neonatal thyroid function in relation to maternal Graves' disease. Best practice & research Clinical endocrinology & metabolism. 2004;18(2):289-302.
7. McLachlan SM, Rapoport B. Thyrotropin-blocking autoantibodies and thyroid-stimulating autoantibodies: potential mechanisms involved in the pendulum swinging from hypothyroidism to hyperthyroidism or vice versa. Thyroid : official journal of the American Thyroid Association. 2013;23(1):14-24.

The terms Pancoast tumors, superior sulcus tumors, and superior pulmonary sulcus tumors are applied to neoplasms located at the apical pleuro pulmonary groove. In 1924, Henry K. Pancoast, described a patient afflicted with a lung carcinoma occupying the apical thoracic cavity that was associated with a constellation of symptoms that included shoulder pain radiating down the arm, atrophy of the hand muscles, and Horner’s syndrome.[ 1] Since then, it has become widely accepted that the term Pancoast syndrome can be applied to any clinical condition in which a neoplasm in the apex of a lung is accompanied by shoulder or arm pain. Anatomically, the definition includes any tumor invading through the parietal pleura at the level of the first rib and above. The pulmonary sulcus refers to the costo vertebral gutter extending from the first rib to the diaphragm. The superior pulmonary sulcus is therefore analogous to the superior most portion of this recess. The first rib is at the base of the thoracic inlet. The thoracic inlet contains the subclavian vein anteriorly, the subclavian artery, phrenic nerve and trunks of the brachial plexus medially, and the nerve roots of the brachial plexus and the stellate ganglion posteriorly. The bony thorax in the superior sulcus includes the upper ribs and the associated vertebral bodies. It is invasion of this complex anatomical area that accounts for the classic symptoms of the Pancoast tumor. Superior sulcus carcinomas have the same biologic behavior as lung carcinomas located in the lung parenchyma. Consequently, their diagnosis, staging, and treatment follow the same principles as for any other lung cancer. The unique characteristics of Pancoast tumors are related to the anatomy of the region where these tumors occur (thoracic inlet) and not to their biologic behavior.
Epidemiology
Pancoast tumors are a relatively rare subset of non-small cell lung cancers (NSCLC), accounting for fewer than 5% of all lung cancers. At least 50% of cases are histologically seen as adenocarcinomas, while the rest are squamous cell and large-cell carcinomas. Small cell carcinoma occurs rare. Patients often present with complaints of pain distributed to the upper anterior chest wall. These tumors may manifest with signs and symptoms related to the compression or infiltration of the middle and lower trunks of the brachial plexus such as shoulder and arm pain (in the distribution of the C8, T1, and T2 dermatome). The peripheral location of these tumors minimizes standard lung cancer symptoms such as cough, hemoptysis, and dyspnea and is the main reason why patients with Pancoast tumors present at a later stage of diagnosis . Diagnosis is established through biopsy of the mass. Given their location, these lesions are amenable to CT or ultrasound-guided fine-needle aspiration. Because of the peripheral location of the tumor, fiberoptic bronchoscopy is only able to establish the diagnosis in less than 30% of cases (unless there is nodal involvement). A tissue diagnosis via video-assisted thoracoscopy (VATS) may be indicated when other investigations are negative and to eliminate the possibility of pleural metastatic disease. Axillary minithoractomy is an alternative to VATS to obtain a tissue diagnosis of the mass in small apical tumors.
As with other lung carcinomas located in the lung parenchyma, it is imperative to stage the mediastinum with Pancoast tumors. Metastases to the mediastinal nodes is a major negative prognostic factor — 5-year survival rates in the presence of N2 disease are below 10%.4 According to the 2013 ACCP guidelines, before surgery for Pancoast tumors, an endobronchial ultrasound with transbronchial needle aspiration or a cervical mediastinoscopy is warranted to exclude N2/N3 disease, even in the absence of involved nodes in CT or PET scans. Pancoast tumors are by definition T3 or T4 tumors. Most of the lesions are classified as T3 tumors because they invade only the chest wall and/or the sympathetic chain. The rest invade brachial plexus, vertebral bodies, and vascular structures, and are classified as T4 tumors. According to the new staging system for lung cancer developed by the International Association for the Study of Lung Cancer (IASLC), their final stage, in the absence of distant metastases, depends on the N status of the tumor:
IIB if T3NO,
IIIA if T3N1-2, or T4NO-1,
IIIB if T3N3 or T4N2-3.
Therefore, even the earliest of these lesions are staged at least IIB. Invasion of the ipsilateral supraclavicular nodes in the setting of lung cancer is classified as N3 disease. In superior sulcus carcinomas the importance of supraclavicular node involvement is quite different because it is considered to represent a locoregional lymph node extension.

References
1] Pancoast H.K. Superior pulmonary sulcus tumor. JAMA. 1932;99:1391.

Dear Editor,
We read with interest the report in the present Journal of Edington M. et al [1] titled “Prescribing lessons from an ocular chemical injury: Vitaros inadvertently dispensed instead of VitA-POS”.
Erectile disfunction drugs play a role increasing levels of cyclic guanosine monophosphate (cGMP) with subsequent effects on nitric-oxide release. This condition can lead to acute angle-closure glaucoma (AACG) in case of anatomical predisposition. AACG is an ophthalmic emergency, it can lead to irreversible blindness if not identified and treated immediately and precipitating factors include certain drugs as nitrates, bronchodilators, cough mixtures, cold and flu medication, antidepressants, antihistamines and anticonvulsants [2]. Furthermore, a precedent case of AACG following sildenafil citrated therapy is also described [3].
We would like underline that this situation could lead to more serious effects, that only the mild chemical ocular injury, in presence of ophthalmic structural diseases.

References:
1. Edington M, Connolly J, Lockington D. Prescribing lessons from an ocular chemical injury: Vitaros inadvertently dispensed instead of VitA-POS. BMJ Case Rep. 2018 Dec 3;11(1). doi: 10.1136/bcr-2018-227468.
2. Murray D. Emergency management: angle-closure glaucoma. Community Eye Health. 2018;31(103):64.
3. Ramasamy B, Rowe F, Nayak H, Peckar C, Noonan C. Acute angle-closure glaucoma following sildenafil citrate-aided sexual intercourse. Acta Ophthalmol Scand. 2007; 85: 229-230.